United States Securities and Exchange Commission Washington, D.C. 20549 FORM 10-K |X| ANNUAL REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934 for the fiscal year ended March 31, 2004. |_| TRANSITION REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934 for the transition period from [___] to [___]. Commission file number 000-25669 IMMTECH INTERNATIONAL, INC. (Exact Name of Registrant as Specified in Its Charter) Delaware 39-1523370 ------------------------------------- --------------------------------------- (State or Other Jurisdiction of (I.R.S. Employer Identification Incorporation or Organization) No.) 150 Fairway Drive, Suite 150, Vernon Hills, Illinois 60061 ------------------------------------- --------------------------------------- (Address of Principal Executive (Zip Code) Offices) Registrant's telephone number, including area code: (847) 573-0033 Securities registered pursuant to Section 12(b) of the Act: None ------------------------ (Title of class) Securities registered pursuant to Section 12(g) of the Act: Common Stock, par value $0.01 per share --------------------------------------------- (Title of class) Indicate by check mark whether the registrant (1) has filed all reports required to be filed by Section 13 or 15(d) of the Securities Exchange Act of 1934 during the past 12 months (or for such shorter period that the registrant was required to file such reports), and (2) has been subject to such filing requirements for the past 90 days. Yes |X| No |__| Indicate by check mark if disclosure of delinquent filers pursuant to Item 405 of Regulation S-K (ss.229.405 of this chapter) is not contained herein, and will not be contained, to the best of registrant's knowledge, in definitive proxy or information statements incorporated by reference in Part III of this Form 10-K or any amendment to this Form 10-K. |X| Indicate by check mark whether the registrant is an accelerated filer (as defined in Rule 12b-2 of the Act). Yes |X| No |_| The aggregate market value of our common stock held by non-affiliates of the registrant, computed by reference to the price at which the common equity was sold, or the average bid and asked price of such common stock as of June 10, 2004, was $103,098,976. As of June 10, 2004, the total number of shares of the registrant's common stock outstanding was 9,905,324 shares. DOCUMENTS INCORPORATED BY REFERENCE ----------------------------------- None. IMMTECH INTERNATIONAL, INC. TABLE OF CONTENTS Page ---- PART I. ITEM 1. BUSINESS.........................................................1 RISK FACTORS ITEM 2. PROPERTIES......................................................41 ITEM 3. LEGAL PROCEEDINGS...............................................42 ITEM 4. SUBMISSION OF MATTERS TO A VOTE OF SECURITY HOLDERS.............43 PART II. ITEM 5. MARKET FOR REGISTRANT'S COMMON EQUITY AND RELATED STOCKHOLDER MATTERS.............................................43 ITEM 6. SELECTED FINANCIAL DATA.........................................49 ITEM 7. MANAGEMENT'S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATIONS.......................................53 ITEM 7A. QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK......64 ITEM 8. FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA.....................64 ITEM 9. CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND FINANCIAL DISCLOSURE........................................64 ITEM 9A CONTROLS AND PROCEDURES.........................................64 PART III. ITEM 10. DIRECTORS AND EXECUTIVE OFFICERS OF THE REGISTRANT..............65 ITEM 11. EXECUTIVE COMPENSATION..........................................69 ITEM 12. SECURITY OWNERSHIP OF CERTAIN BENEFICIAL OWNERS AND MANAGEMENT......................................................72 ITEM 13. CERTAIN RELATIONSHIPS AND RELATED TRANSACTIONS..................75 ITEM 14. PRINCIPAL ACCOUNTANT FEES AND SERVICES..........................76 PART IV. ITEM 15. EXHIBITS, FINANCIAL STATEMENT SCHEDULES AND REPORTS ON FORM 8-K.............................................................77 FORWARD-LOOKING STATEMENTS Certain statements contained in this annual report and in the documents incorporated by reference herein constitute "forward-looking statements" within the meaning of the Private Securities Litigation Reform Act of 1995. All statements other than statements of historical fact may be deemed to be forward-looking statements. Forward-looking statements frequently, but not always, use the words "intends," "plans," "believes," "anticipates" or "expects" or similar words and may include statements concerning our strategies, goals and plans. Forward-looking statements involve a number of significant risks and uncertainties that could cause our actual results or achievements or other events to differ materially from those reflected in such forward-looking statements. Such factors include, among others described in this annual report, the following: (i) we are in an early stage of product development, (ii) the possibility that favorable relationships with collaborators cannot be established or, if established, will be abandoned by the collaborators before completion of product development, (iii) the possibility that we or our collaborators will not successfully develop any marketable products, (iv) the possibility that advances by competitors will cause our product candidates not to be viable, (v) uncertainties as to the requirement that a drug product be found to be safe and effective after extensive clinical trials and the possibility that the results of such trials, if completed, will not establish the safety or efficacy of our drug product candidates, (vi) risks relating to requirements for approvals by governmental agencies, such as the Food and Drug Administration, before products can be marketed and the possibility that such approvals will not be obtained in a timely manner or at all or will be conditioned in a manner that would impair our ability to market our product candidates successfully, (vii) the risk that our patents could be invalidated or narrowed in scope by judicial actions or that our technology could infringe upon the patent or other intellectual property rights of third parties, (viii) the possibility that we will not be able to raise adequate capital to fund our operations through the process of commercializing a successful product or that future financing will be completed on unfavorable terms, (ix) the possibility that any products successfully developed by us will not achieve market acceptance and (x) other risks and uncertainties that may not be described herein. We undertake no obligation to update or revise any forward-looking statements, whether as a result of new information, future events or otherwise. PART I ITEM 1. BUSINESS A. Business Overview Immtech International, Inc. is a pharmaceutical company advancing the development and commercialization of oral drugs to treat infectious diseases, and metabolic (diabetes) and neoplastic (cancer) disorders. We have drug development programs that include treatments for fungal infections, malaria, tuberculosis, diabetes, Pneumocystis carinii pneumonia ("PCP") and tropical medicine diseases, including African sleeping sickness (trypanosomiasis) and leishmaniasis. We recently signed an agreement with CombinatoRX, Inc. to evaluate our first drug DB289 (in combination with other drugs on the market) for anticancer activity; currently CombinatorRX is using a drug similar in structure to DB289 as a combination partner in Phase II clinical trial for the treatment of solid tumors. We hold worldwide patents and patent applications, and licenses and rights to license technology, primarily from a scientific consortium that has granted us exclusive rights to commercialize products from, and license rights to, the technology. Our scientific consortium includes scientists from The University of North Carolina at Chapel Hill ("UNC"), Georgia State University ("Georgia State"), Duke University ("Duke University") and Auburn University ("Auburn University") (collectively, the "Scientific Consortium"). Our strategy is to develop oral drugs effective against infectious diseases and metabolic and neoplastic disorders utilizing a dicationic technology platform. Infectious diseases in the global population have increased significantly during the past 20 years and are the most common cause of death worldwide according to the World Health Organization ("WHO"). Relatively few new drugs for treatment of infectious diseases have been brought to market during this period. New antibiotics are needed to overcome the problems of multi-drug resistance and the increasing number of new pathogens that are causing diseases in the world. Metabolic and neoplastic disorders, including diabetes and cancer, cause illness and death worldwide. Scientists have struggled for decades to find effective treatments for both diabetes and cancer. Our initial in vitro studies have demonstrated that the dication platform is effective against these two devastating diseases. Since our formation in October 1984, we have engaged in pharmaceutical research and drug development, expanding our scientific capabilities and collaborative network, developing technology licensing agreements, and advancing the commercialization of our proprietary technologies, including the development of aromatic cations (which includes dications) commencing in 1997. In addition to our internal resources, we use the expertise and resources of strategic partners and third parties in a number of areas, including (i) discovery research, (ii) pre-clinical and human clinical trials and (iii) manufacture of pharmaceutical drugs. We intend to work with our scientific and foundation partners to validate our technology platform, illustrating dications' low toxicity, broad application, and oral deliverability. We plan in the near future to sell drugs for compassionate use in niche markets as we further develop drugs to target multi-billion dollar markets such as antifungal, TB, diabetes and cancer treatments. As a validation of our efforts, the United States Food and Drug Administration ("FDA") has granted "fast-track" designation to DB289 for treatment of African sleeping sickness. Fast-track designation allows for expedited FDA regulatory review of DB289 for African sleeping sickness. For the fiscal year ended March 31, 2004, we had revenues of approximately $2,416,000 and a net loss of $12,846,000 which consisted primarily non-cash compensation expense related to the vesting of common stock options and warrants issued during the year which was approximately $7,501,000. Our management believes we have sufficient capital for operations through our next fiscal year. There is no guarantee that we will not need additional funds before then or that sufficient funds will be available after April 2005 to fund further operations. A predecessor of our Company was incorporated under the laws of the State of Wisconsin on October 15, 1984, and subsequently merged into the current Delaware corporation on April 1, 1993. Our executive offices are located at 150 Fairway Drive, Suite 150, Vernon Hills, Illinois 60061, telephone number (847) 573-0033 or toll-free (877) 898-8038. Our common stock is listed on The American Stock Exchange under the ticker symbol "IMM". Trading on the AMEX commenced on August 11, 2003. -2- We file annual, quarterly and current reports, proxy statements and other documents with the United States Securities and Exchange Commission (the "SEC"), under the Securities Exchange Act of 1934, as amended (the "Exchange Act"). You may read and copy any materials that we file with the SEC at the SEC's Public Reference Room at 450 Fifth Street, N.W., Washington, D.C. 20549. You may obtain information on the operation of the Public Reference Room by calling the SEC at 1-800-SEC-0330. Our reports, proxy statements and other documents filed electronically with the SEC are available at the website maintained by the SEC at http://www.sec.gov. We also make available free of charge on or through our Internet website, http://www.immtech-international.com, our annual, quarterly and current reports, and, if applicable, amendments to those reports, filed or furnished pursuant to Section 13(a) of the Exchange Act, as soon as reasonably practicable after we electronically file such reports with the SEC. Information on our website is not a part of this report. Generally, when we use the words "we," "our," "us," the "Company" or "Immtech" in this report, we are referring to Immtech International, Inc. and its subsidiaries. B. Products and Programs We currently have three human clinical trials and several more laboratory development programs underway testing the effectiveness of DB289 for various indications. We are able to coordinate the development of simultaneous treatment programs by building on the results of our African sleeping sickness Phase IIb safety and efficacy trial which allowed the Company to initiate Phase II studies in malaria and PCP. Dosage and treatment regimen for certain indications vary in each trial; however, our safety data from Phase I and II trials for DB289 have allowed us to expedite development of the dication technology into new treatment areas. 1. Malaria Malaria is the second most deadly infectious disease in the world and is a significant problem for over 2.4 billion people exposed to this mosquito-borne disease. Malaria affects 300 to 500 million people each year and is especially devastating to children under the age of five for whom the fatality rate is very high. It is estimated by the World Health Organization (the "WHO") that over a million children die every year from malaria. The Global Fund to Fight AIDS, Tuberculosis and Malaria and Medicines for Malaria Venture ("MMV"), both foundations supported by The Bill and Melinda Gates Foundation ("The Gates Foundation"), are supporting the development of new oral drugs for safe and effective treatment of patients with drug-resistant forms of malaria. In November 2003, we received a grant of approximately $668,000 from MMV to fund clinical studies and manufacturing of DB289 for treatment of malaria. Subject to reaching certain milestones, MMV has committed approximately $8.2 million to fund further clinical testing of DB289 to treat malaria and to commercially license its use. In June 2003, we commenced and completed a Phase IIa clinical trial of DB289 targeting two strains of the malaria parasite (Plasmodium vivax and Plasmodium -3- falciparum, the two most common human forms of malaria in the world). Our pre-clinical data and pharmacokinetics (pharmacokinetics is the study of the uptake, distribution and rate of movement of a drug in the body from the time it is absorbed until it is eliminated) studies conducted in humans indicated that sufficient levels of DB289 could be reached in the blood to effectively treat malaria in humans. DB289 demonstrated positive activity against several non-human forms of malaria (used as surrogates for the human disease) in animal models of the disease. DB289 also showed positive activity in vitro against known drug-resistant strains of malaria, including chloroquine-resistant strains of malaria. Chloroquine is the drug most frequently used to treat malaria in developing countries. In December 2003, we reported the results of the Phase IIa malaria trial that was conducted in Thailand. The patients who participated in the malaria trial were treated with 100 mg capsules of DB289 twice per day for five consecutive days. All 32 patients treated cleared the malaria parasite and malaria symptoms (i.e., fever) disappeared quickly within the five-day treatment period; 50% of the patients cleared the malaria parasite within 24 hours of the first dose. Tolerance to DB289 was excellent with no significant adverse side effects reported. All patients were followed and monitored for 28 days after treatment to ensure that the malaria parasite had been completely eliminated. Out of the 32 patients, nine were infected with Plasmodium vivax and 23 patients with Plasmodium flaciparum (the most deadly form of malaria contracted by humans). P. vivax infected patients usually have less severe symptoms, but reoccurrence is very high and a large percentage develop chronic forms of the disease. P. falciparum has more severe symptoms (including high fever), and causes over 2 million deaths per year. Chloroquine, the most commonly used treatment, has high levels of drug-resistance. The P. falciparum patients were treated with DB289 as a monotherapy (not in combination with any other drugs). Of the 23 patients treated for P. falciparum, the cure rate was approximately 95% as one of the patient had malaria in the 28-day after treatment period. However, blood samples from a second patient reported originally with parasites in the blood at 28 days is now believed (after more extensive testing) to have a new infection. Nine P. vivax patients were treated with DB289 for five days followed by oral Primaquine (drug combination therapy is used as standard therapy for P. vivax treatment). 100% of patients treated with both drugs for P. vivax remained clear of any parasites on the 28th day of the trial without any adverse events or safety issues with the combination therapy. Based on the results of the Phase IIa malaria trial in Thailand, we have initiated several new trials that will begin in July, 2004; (1) a new study in Thailand will evaluate DB289 in combination with Artemisinin, (thereby potentially creating a new drug cocktail to treat malaria) and (2) a study in uninfected, normal volunteers to determine if DB289 can be given at higher (single) doses for three days. In addition, the study in volunteers will include three different ethnic groups to compare metabolism of DB289 and comparing 5 day dosing to 3 day dosing. The combination study is designed to evaluate potential drug interactions between Artemisinin and DB289 in patients with acute to moderate malaria. The study incorporates several dose levels and regimens (once daily -4- versus twice daily dosing) and will be conducted in Thailand. The study design is set forth below. -------------------------------------------------------------------------------- Clinical Trial Trial Design/Phase II End Points Sites -------------------------------------------------------------------------------- DB289 in combination o Oral Dosing 3 days o Drug interactions Thailand with Artemisinin o Artemisinin & o Safety DB289 o Parasite clearance o Clinical improvement a. MMV Agreement ------------- On November 26, 2003, we entered into a Testing Agreement with MMV, a foundation established in Switzerland, and UNC pursuant to which we, with the support of MMV and UNC, are conducting a study of DB289 as a treatment for malaria. The studies to be performed include Phase II and Phase III human clinical trials, and drug development activities of DB289 alone, and in combination with other anti-malarial drugs, with the goal of obtaining regulatory approval of a product for the treatment of malaria. Under the terms of the agreement, MMV has committed to advance funds to the Company to pay for human clinical trials and regulatory preparation and filing costs to obtain approval to market DB289 for treatment of malaria. MMV will pay for regulatory approvals for DB289 in at least one internationally accepted regulatory body and at least one malaria endemic country. We have forecasted such costs to be approximately $8.2 million. MMV has agreed to fund the forecasted amount based on progress achieved. Through the fiscal year ended March 31, 2004, MMV has funded $668,000 for human clinical trials conducted from June to December 2003. Under this agreement, UNC will receive approximately $50,000 for its work to evaluate synergistic qualities of other drugs that may be used in combination with DB289 as a malarial drug "cocktail". b. Related MMV/UNC Agreement ------------------------ In a related "Discovery Agreement" between MMV and UNC, MMV has agreed to fund a research program with a three year budget of approximately $1.4 million. The goals of the Discovery Agreement are to design synthesis and optimize new compounds for testing and evaluation of effectiveness for treatment of malaria. Immtech is a third party beneficiary of the Discovery Agreement and, pursuant to the terms of the Consortium Agreement (defined below), has the rights to develop and commercialize the discoveries resulting therefrom. 2. African Sleeping Sickness (Human trypanosomiasis) African sleeping sickness is a parasitic disease that is spread by tsetse flies in sub-Sahara Africa where 60 million people live. Doctors Without Borders estimates -5- The geographical range in sub-Sahara Africa where human African sleeping sickness occurs encompasses 36 countries, wherein over 60 million persons are at risk of contracting the disease. Existing treatments for African sleeping sickness can be highly toxic and cannot be administered orally. African sleeping sickness is fatal if left untreated. WHO estimates that there are 500,000 to 750,000 active cases of human African sleeping sickness in central Africa. A WHO survey reports that an "epidemic situation" for African sleeping sickness exists in the sub-Sahara region of Africa which includes the countries of Angola, Sudan, Uganda and the Democratic Republic of the Congo ("DRC"). Human African sleeping sickness may take one of two forms depending upon the origin of the parasite that transmits the disease: (1) West African sleeping sickness is caused by Trypanosoma brucei gambiense and (2) East African sleeping sickness is caused by Trypanosoma brucei rhodesiense. Although DB289 has activity in both forms, thus far we have conducted clinical trials of DB289 as a treatment for West African sleeping sickness, the area of sub-Sahara Africa that has an ongoing epidemic. In September 2002, we completed a Phase IIa study of DB289 in the Democratic Republic of Congo ("DRC") for treatment of African sleeping sickness. Initial results showed that the compound was well tolerated and over 95% of the patients treated were cured (patients evaluated three and six months after treatment were still parasite free). Based upon the promising results of the Phase IIa clinical trial, The Gates Foundation made an additional grant of $2.7 million to the UNC Scientific Consortium to accelerate the planned Phase IIb/III clinical trials. In April 2003 we commenced a 350-patient, randomized Phase II/III pivotal human clinical trial to treat African sleeping sickness with DB289. In this randomized clinical trial, half the patients in the study receive DB289 and half the patients receive Pentamidine intramuscular injections (standard first line therapy). The Phase IIb clinical trial commenced in two larger sites in Maluku and Vanga in the DRC where patients receive extensive safety monitoring. We have plans to add three -6- additional sites in remote villages, where we intend to perform a similar level of treatment and patient monitoring. The three added testing sites will permit accelerated patient enrollment rates for the clinical trials. In February 2004 we completed the first 80 patients in the Phase II/III pivotal trial. Patient monitoring included EKG monitoring, blood sampling to check clinical chemistry and hematology parameters and various other clinical measurements and tests, including the clearance of parasites from blood. The results from the initial 80 patients in the pivotal trial continues to show that DB289 is safe to administer to patients. In the patients treated at the Vanga site several patients did not clear the parasite from the lymph nodes. Based on this information, we opened a new arm of the study to test a new dose regimen in 30 patients using DB289 for 10 days (twice daily at 100mg per dose). We expect that the new dose regimen will resolve the clearance of the very small number of parasites found in the lymph nodes. This study should be concluded in August 2004. Once the extended regimen is completed, we plan to open three additional clinical sites, two in the DRC and one in Angola, which we believe will increase enrollment in the trial to 250 patients. (See trial design below). Assuming favorable test results, we believe we will receive a purchase order before the end of 2004 and government approvals to distribute for compassionate use in 2005, DB289 as a treatment for African sleeping sickness in several African countries. We have engaged a large scale pharmaceutical contract manufacturer, Cambrex, Inc., to produce DB289 for the clinical trials and commercial sales. We plan to concurrently with scale-up seek final foreign regulatory approvals to commercially distribute the product into selected countries. All clinical trials of DB289 are being conducted under an Investigational New Drug ("IND") application with the FDA. In addition to an IND filed with the FDA, on April 23 the FDA granted "Fast-Track" drug development designation for use of DB289 to treat human African sleeping sickness. We believe the FDA's Fast-Track designation indicates the FDA's recognition of DB289's potential to safely treat this life-threatening disease for which no other oral treatment exists. Our studies have demonstrated DB289's effectiveness to safely treat human African sleeping sickness without the serious side effects associated with alternative (non-orally deliverable) therapies. Fast-Track designation also allows DB289 to be eligible for expedited FDA licensing review assuming test results continue as expected. Our data to date suggests that DB289 can safely and effectively treat human African sleeping sickness without the serious side effects associated with alternative (non-orally deliverable) therapies currently used in Africa. Oral delivery is particularly important in remote geographic areas where this disease is endemic and without access to hospitals or clinics which are needed to deliver the current therapy. -7- Our pivotal clinical trial design for using DB289 to treat human African sleeping sickness is set forth below: --------------------------------------------------------------------------------------------------------------- Clinical Trial Trial Design / Phase Expected Result Sites --------------------------------------------------------------------------------------------------------------- DB289 Pivotal Trial o African sleeping o Phase III o Safety o Democratic sickness o 250 patients - stage 1 o Clearance of Republic of disease parasite from blood the Congo o Oral dosing for 5 to 10 after treatment and (4 sites) days (BID) 3, 6 months o Randomized comparison to o Improvement of o Angola (1 site) pentamidine symptoms a. Gates Grant ----------- In November 2000, The Gates Foundation awarded a $15.1 million grant to a research group led by UNC to develop new drugs to treat African sleeping sickness and leishmaniasis, two life-threatening diseases endemic in sub-Sahara Africa. The research group led by UNC includes Immtech and five other universities and research centers around the world which collectively employ scientists and physicians considered to be the foremost experts in one or both of these diseases. b. Gates Acceleration Grant ------------------------ In June 2003, the Gates Foundation awarded an additional $2.7 million grant to the UNC led research group to (i) expand ongoing Phase IIb/III clinical trials of DB289 for treatment of African sleeping sickness by adding additional clinical sites and increasing patient enrollment in several sub-Sahara African nations, (ii) implement an improved method of synthesizing DB289 to reduce drug manufacturing costs and (iii) improve DB289's formulation to facilitate increased drug delivery concentration in blood circulation. Pursuant to the terms of the Clinical Research Subcontract described below, ninety-one percent of this grant ($2,466,475) is directed to Immtech. On June 26, 2003 we received $1,025,201 to advance the goals set forth above. c. Clinical Research Subcontract with UNC -------------------------------------- On March 29, 2001, we entered into a clinical research subcontract ("Clinical Research Subcontract") with UNC to advance the work funded by The Gates Foundation $15.1 million grant. Pursuant to the Clinical Research Subcontract, UNC is to pay to us $9.8 million of the $15.1 million grant in installments over a period not to exceed five years based on our achieving certain milestones (approximately $7.7 million of which has been paid to us to date). Under the terms of the Clinical Research Subcontract, we are responsible for the oversight of Phase II and Phase III human clinical trials of the drug candidate DB289 for African sleeping sickness. The terms of the Clinical Research Subcontract require us to segregate the Clinical Research Subcontract funds from our other funds and to use the proceeds only for developing a drug for treatment -8- of African sleeping sickness. We have or will receive The Gates Foundation grant funds under the Clinical Research Subcontract as follows: (a) $4.3 million was received in fiscal year 2001 to fund Phase II clinical trials to test DB289's effectiveness against African sleeping sickness in approximately 30 patients, (b) $1.4 million was paid to us in September 2002 upon the successful completion of our Phase IIa clinical trial, (c) $2.0 million was paid to us in December 2002 upon the delivery of the final Phase IIa report in respect of the Phase II clinical trial and (d) $2.1 million is scheduled to be paid in June 2004 to fund Phase IIb and Phase III clinical trials which have been commenced to test compound DB289's effectiveness against African sleeping sickness on a larger, more diverse group of patients in calendar year 2005. The Clinical Research Subcontract will continue in effect until November 17, 2005, unless otherwise terminated by a material breach by either party. 3. PCP pneumonia In 2002, we received approval from the U.S. FDA and the Ministry of Health in Peru to commence a pilot Phase IIa clinical trial of DB289 to treat Pneumocystis carinii pneumonia ("PCP"). PCP is a fungus that overgrows the air sacs in the lungs of immunosuppressed patients, causing pneumonia that can be life-threatening. A proof of concept trial in 8 immunosuppressed patients that had failed standard therapy were given 50 mg of DB289 for 21 days; the treatment was completed in February, 2003. The results from the study demonstrated that DB289 was safe and effective in all of the AIDS patients. All patients showed improved lung function. In the 21 days of treatment, three of the patients were able to return to normal lung function. A second Peruvian trial is underway using a dosage of 100 mg twice per day (a higher dose than the pilot study) in 30 patients. The initial data from 19 patients who have completed the trial indicates that all patients returned to normal lung function within 12 days. The higher dosage regimen appears to significantly increase the number of patients that clear the infection (demonstrate lung function improvement) and decreased the time to cure the patients. All patients selected for the Phase IIb trial were AIDS patients who had previously failed other therapies used to treat PCP. Our current clinical trial protocol for testing of DB289's effectiveness against PCP is set forth below: -9- ------------------------------------------------------------------------------------------------ Clinical Trial Trial Design / Phase Expected Result Sites ------------------------------------------------------------------------------------------------ DB289 o PCP o Phase IIa o Safety o Peru o Patients who failed o Improvement in lung standard treatment function (fungal o Oral dosing for 21 days clearance) o Twice daily dosages of o Improvement in 100mg clinical symptoms 4. Antifungal Program Scientific Consortium scientists from Duke University, UNC and Georgia State have identified several compounds with the potential to treat both Candida and Aspergillus, two fungal infections that in the aggregate account for approximately 90% of the systemic fungal infection that make up the $4 billion annual drug market (as estimated by DataMonitor). In vitro laboratory studies have identified over 20-30 dications that display both broad based and selective antifungal activity against Candida, Aspergillus and Cryptococcus, including activity against fungi which had previously been shown to be drug resistant. Our objective in 2004 is to select an oral drug candidate for the treatment of fungal infections and begin preclinical safety and pharmacology studies required prior to human trials. The market for an effective antifungal drug was estimated in 2003 to be approximately $4 billion annually and growing rapidly due to the increasing number of patients who are susceptible to fungal diseases, such as patients undergoing cancer chemotherapy, patients with HIV and those who have undergone organ transplants. In addition, the frequency of nosocomial infection (infection acquired while being treated in a hospital) caused by fungi has increased drastically and is now the third most common cause of sepsis, replacing Escherichia coli ("E. coli"). Sepsis is an infection that quickly overwhelms the immune system and can lead to sudden death. Recently, strains of fungi have developed that are resistant to currently available treatments. There is a significant opportunity for new oral effective against specific strains of fungi as well as drugs with broad spectrum effectiveness across fungal strains. Duke University researchers have developed an animal model of Candida and Aspergillus and are testing compounds in this model. In addition, the Company has a contract with Case Western University ("Case Western") to test lead compounds in animal models of fungal infections. Case Western is evaluating dose responses for a number of our compounds to determine which will be the best compound to move forward into preclinical development. 5. Tuberculosis Tuberculosis ("TB") is the world's number one killer among infectious diseases and is the cause of over two million deaths per year, according to the WHO and -10- the U.S. Centers for Disease Control (the "CDC"). The CDC reports that about two billion people, including fifteen million Americans, are infected with TB. The disease is spreading rapidly in developing countries in Asia, Africa and South America, and is becoming increasingly problematic in developed countries and in Eastern Europe. Japan has declared TB as its most threatening disease. An alarming increase in TB cases is also developing in the United States. The combination of the rapid spread of TB and the appearance of multi-drug resistant strains ("MDR") of the TB organism make TB a major health threat throughout the world. TB is a difficult infection to treat given that the bacteria is often sequestered in various tissues and organs of the body. The organisms that cause the disease can "hide" inside white blood cells where the organisms are protected against antibiotic drugs. To be effective, a drug must eliminate the TB organisms from the lungs, tissues, and infected white blood cells. WHO and the National Institutes of Health ("NIH") have significantly increased research efforts to discover drugs to treat TB. Their research is focused on developing oral drugs that are effective against drug resistant strains of TB and the creation of therapies to shorten the treatment period required to eradicate the disease. Their overall target is to reduce the current nine- to eighteen-month treatment period down to two- to six- months. NIH laboratories screened over 500 of our dication compounds looking for potential drug candidates for treatment of TB. The NIH screening program identified approximately 10 to 15 dications with in vitro activity comparable or superior in performance to drugs currently available to treat TB. We moved our screening and animal testing program to the University of Illinois-Chicago ("UIC") which is directed by Dr. Scott G. Franzblau, to develop new drugs to combat the common and MDR strains of Mycobacterium TB. Dr. Franzblau is a leading expert in TB treatment. Prior to running the TB program at UIC, Dr. Franzblau led the NIH-funded anti-TB screening program at the National Hansen's Disease Center at Louisiana State University. The in vitro screening program at UIC identified seven new compounds which displated excellent activity which have been selected for in vivo screening. The UIC laboratory is evaluating these newly identified compounds and several from the NIH screening program in acute and latent animal models of TB. We believe that the final test results will assist us in selecting a compound this year that will move into pre-clinical studies required prior to human trials. 6. Pharmaceutical Cancer Program We have provided under a confidentiality, material transfer and testing agreement with CombinatoRx of Boston, Massachusetts certain of our aromatic cationic compounds, including DB289 and DB75, to be tested for activity against certain cancers. CombinatoRx previously tested various combinations of drugs not normally associated with cancer treatments for effectiveness against cancer and has had promising results. Several of our aromatic dication compounds have similar medicinal properties to those used by CombinatoRx in its earlier tests. Our compounds, however, do not have the adverse side-effects and delivery difficulties generally associated with those other pharmaceuticals tested by CombinatoRx. We and CombinatoRx believe that our -11- aromatic cationic compounds' broad-based activities and unique mechanism of action will demonstrate, through CombinatoRx's studies, activity in oncology. CombinatoRx's studies will include in vitro assays and in vivo models and will test our compounds in combination with CombinatoRx's proprietary anti-cancer technology. C. Technology 1. Dications Our pharmaceutical program focuses on the development and commercialization of oral drugs to treat fungal, parasitic, bacterial and viral diseases and certain metabolic and neoplastic disorders, including diabetes and cancer. Aromatic dications are chemical structures that have two positively charged ends that are held together by a linker; at the atom level, they look like molecular barbells. In addition, a new class of monocations have been made with excellent activity in specific target diseases, these compounds have a single positive charge on one end and a linker. The positive charges as one mechanism of action allow our compounds to bind to negatively charged segments of deoxyribonucleic acid ("DNA"). Dication drugs bind in the minor groove of DNA and to certain receptors, blocking the activity of enzymes needed for microbial growth. The key site on an organism's DNA is an area where enzymes interact with the organism's DNA as part of their normal life cycle. Structurally, dications are chemical molecules that have two positively charged ends held together by a chemical linker. The composition of the dications, with positive charges on the ends and linkers of different length, shape and binding curvature allows specific dication binding and hence, anti-microbial activities. Pentamidine (a dicationic drug on the market) was the prototype drug used by scientists at UNC to develop our proprietary library of aromatic compounds. While having broad based activity against many diseases including fungal infections and cancer, pentamidine can only be administered intravenously, by intramuscular injection, or via inhalation. Pentamidine is difficult and costly to administer outside of a hospital setting due to its narrow therapeutic dosage margin of safety and efficacy. Scientists at UNC discovered that much of pentamidine's toxicity was the result of bi-products formed when the drug breaks down within the body. This discovery by the scientists led to the design of new compounds which did not break down in the same way. Additional modifications to the structures of these compounds improved on their binding activity and enhanced the applicability of this class as antibiotics over other anti-infectious agents, while lowering toxicity and increasing oral deliverability. Scientific Consortium members have thus far designed and synthesized over 2,200 well-defined aromatic cationic compounds. These compounds have all been tested in a wide variety of assays and animal models of various diseases. UNC and Georgia State continue to improve methods for making cationic molecules in computer models that help to develop medicinally efficacious compounds. One or more of the universities comprising the Scientific Consortium have patents covering the molecular structure of -12- the compounds, as well as in some cases particular uses of a compound for potential treatment of an infection or disease. Members of the Scientific Consortium have laboratory testing systems for screening dications for activity against specific microorganisms (using both laboratory and animal models). Our scientists have over 25 years of experience in making dication compounds and have developed proprietary computer models which help our scientists rationally design the next generation of compounds. Generally, patents for the aromatic cation structures and uses are issued to the scientist who invents or discovers the new compound and/or proves its unique applicability for particular diseases. Then, pursuant to the scientist's employment arrangements, the patents are assigned to the employing university, and, through the License Agreement (see 2, The Scientific Consortium, a Consortium Agreement and License below), to us through an exclusive worldwide license to commercialize such compounds and uses. a. DB289 ----- DB289 is an aromatic dication that utilizes Prodrug oral delivery technology to deliver the active drug into blood circulation by swallowing a pill. In May 2001, we completed Phase I safety trials of DB289 in human volunteers. The single and multi-dose trials demonstrated that DB289 was well tolerated by the volunteers. The study was designed to evaluate the safety and pharmacokinetics (pharmacokinetics is the study of a drug's effect on the body from the time it is absorbed until it is eliminated) of three dosage levels of DB289 administered twice a day over a period of six days. In addition to the safety studies. The volunteers who were given the active drug participated in a secondary study to determine whether food affected absorption through the digestive system. The studies showed that DB289 passed easily through the digestive membrane and the drug was active (as designed) for several hours in the bloodstream. In addition, volunteers tested at the highest dosage levels in the multi-dose segment of the trial did not display any specific side effects, and the post-test EKGs, clinical chemistry and hematology parameters of those volunteers were all within normal ranges. The drug concentration levels in the blood were similar to levels that showed effectiveness in animal models in malaria, PCP and African sleeping sickness. In 2002 we began human trials in patients infected with the Trypanosome parasite that causes African sleeping sickness (see page 6). b. Prodrug Formulation ------------------- One of our most significant research developments was the discovery of technology to make dication drugs orally deliverable. This proprietary technology temporarily masks the positive charges of the dication, enabling the active compound to move easily across digestive membranes into blood circulation. Once the drug is in blood circulation, the masking charges are removed by naturally occurring enzymes thereby releasing the active drug. Until -13- now, the inability to deliver active compounds across the digestive membrane into the bloodstream had reduced the attractiveness of aromatic cations/dications as effective antibiotics. Our scientists have patented four Prodrug synthesis methods allowing for oral delivery and making this entire class of compounds significantly more attractive for commercial development. On February 26, 2003, Scientific Consortium members were granted a patent by the U.S. Patent Office entitled "Prodrugs for Antimicrobial Amidines" for a new proprietary technology to synthesize and manufacture dication and other compounds with Prodrug technology. This patent protects a substantially advanced process for economically producing oral drugs designed to treat infectious diseases and metabolic disorders such as fungal infections, malaria, tuberculosis, diabetes, Pneumocystis carinii pneumonia and tropical medicine diseases, including African sleeping sickness (trypanosomiasis) and leishmaniasis. Application of Prodrug technology is not limited to our products, and we are investigating the potential to sub-license the Prodrug process to other drug manufacturers for use on other compounds designed to be ingested orally and then activated in the blood stream. 2. The Scientific Consortium The Scientific Consortium responsible for the invention and development of dication technology includes scientists from UNC, Georgia State, Duke University and Auburn University (collectively, the "Scientific Consortium"). a. Consortium Agreement and License -------------------------------- On January 15, 1997, we entered into a Consortium Agreement with UNC and Pharm-Eco Laboratories, Inc. ("Pharm-Eco") (to which each of Georgia State, Duke University and Auburn University agreed shortly thereafter to become a party). The Consortium Agreement provided that dications developed by the Scientific Consortium-members were to be exclusively licensed to us for global commercialization. As contemplated by the Consortium Agreement, on January 28, 2002, we entered into a License Agreement with the Scientific Consortium whereby we received the exclusive license to commercialize all future technology and compounds ("future compounds") developed or invented by one or more of the Scientific Consortium scientists after January 15, 1997, and which also incorporated into such License Agreement our license with the Scientific Consortium with regard to compounds developed on or prior to January 15, 1997 ("current compounds"). Pursuant to the Consortium Agreement, Pharm-Eco agreed to transfer to us the worldwide exclusive license to use, manufacture, have manufactured, promote, sell, distribute or otherwise dispose of any and all products based directly or indirectly on dications developed by the Scientific Consortium on or prior to January 15, 1997 and previously licensed (together with related technology and patents) to Pharm-Eco. In March 2001, Pharm-Eco -14- assigned the license to us. The January 28, 2002, License Agreement grants to us a similar worldwide exclusive license covering products based on dicationic technology developed by the Scientific Consortium after January 15, 1997 and incorporates the exclusive license assigned to us by Pharm-Eco in March 2001. The Consortium Agreement has provided us with rights to the Scientific Consortium's library of over 2,000 well-defined aromatic cationic compounds/dications and to all future technology to be designed by the Scientific Consortium. The Scientific Consortium scientists are considered to be among the world's leading experts in infectious diseases, computer modeling of dicationic pharmaceutical drugs and computer-generated drug designs. The Consortium Agreement provides that we are required to pay to UNC on behalf of the Scientific Consortium reimbursement of patent and patent-related fees, certain milestone payments and royalty payments based on revenue derived from the Scientific Consortium's dication technology. Each month on behalf of the inventor scientist or university, as the case may be, UNC submits to us an invoice for payment of patent-related fees related to current compounds or future compounds incurred prior to the invoice date. For the fiscal year ended March 31, 2004, we reimbursed UNC $473,567 for such patent and patent-related costs, and in the past, we have reimbursed to UNC approximately $1,413,000 in the aggregate in patent and patent-related costs. We are also required to make milestone payments in the form of issuance of 100,000 shares of its common stock to the Consortium when we file our initial New Drug Application ("NDA") or an Abbreviated New Drug Application ("ANDA") based on Consortium technology and are required to pay to UNC on behalf of the Scientific Consortium (other than Duke University) (i) royalty payments of up to 5% of our net worldwide sales of "current products" and "future products" (products based directly or indirectly on current compounds and future compounds, respectively) and (ii) a percentage of any fees we receive under sublicensing arrangements. With respect to products or licensing arrangements emanating from Duke University technology, we are required to negotiate in good faith with UNC (on behalf of Duke University) royalty, milestone or other fees at the time of such event, consistent with the terms of the Consortium Agreement. Under the License Agreement, we must also reimburse the cost of obtaining patents and assume liability for future costs to maintain and defend patents so long as we choose to retain the license to such patents. D. Our Subsidiaries 1. Immtech Hong Kong Limited On January 13, 2003, we entered into an agreement with an investor who owned, through Lenton Fibre Optics Development Limited ("Lenton"), a Hong Kong company, a 1.6+ acre commercial real estate parcel located in a "free-trade zone" called the Futian Free Trade Zone, Shenzhen, in the People's Republic of China ("PRC"). Under the agreement, we purchased an 80% interest in Lenton by issuing to the investor -15- 1,200,000 unregistered shares of our common stock, $0.01 par value. We subsequently resold to the investor our interest in Lenton and the parcel of land in exchange for 100% ownership in the improved property described below under Super Insight Limited and Immtech Life Science Limited. In connection with the sale of Lenton, we acquired 100% ownership of Immtech Hong Kong Limited ("Immtech HK"), including Immtech HK's interest in Immtech Therapeutics Limited. Subsequently, though a sublicense agreement, we transferred to Immtech HK our rights to develop and license university technology in certain Asian countries and to commercialize resulting products granted to us under the Consortium Agreement. We intend to use Immtech HK as a vehicle to further sublicense rights to develop specific indications to our indirect subsidiaries that will partner with investors who fund development costs of those indications. Immtech HK is a Hong Kong company. a. Immtech Therapeutics Limited ---------------------------- Immtech Therapeutics Limited ("Immtech Therapeutics") provides assistance to healthcare companies seeking access to China to conduct human clinical trials and to manufacture and/or distribute pharmaceutical products in China. Immtech Therapeutics is majority owned by Immtech HK and its minority owners are Centralfield International Limited (a British Virgin Island (BVI) company and wholly-owned subsidiary of TechCap Holdings Limited) and Bingo Star Limited (BVI). TechCap has assets and resources in China upon which Immtech Therapeutics may draw. Bingo Star Limited has substantial financial and medical expertise and resources located in Hong Kong and China. Immtech Therapeutics is a Hong Kong company. 2. Super Insight Limited (BVI) On November 28, 2003, we purchased from an investor 100% of Super Insight Limited ("Super Insight") and its wholly-owned subsidiary, Immtech Life Science Limited ("Immtech Life Science") and (ii) from Lenton Fiber Optics Development Limited, a 100% interest in Immtech HK. As payment for the acquisition, we transferred to the investor our 80% interest in Lenton and cash. Super Insight is a British Virgin Islands company. a. Immtech Life Science Limited ---------------------------- Immtech Life Science owns two floors of a newly-constructed building (the "Property") located in the Futian Free Trade Zone, Shenzhen, in the PRC in which Immtech intends to house a pharmaceutical production facility for manufacture of its products. The Property comprises Level One and Level Two of a building named the Immtech Life Science Building. The duration of the land use right associated with the building on which the Property is located is 50 years which expires May 24, 2051. -16- Under current law, we will enjoy reduced tax on the business located on the Property because the local government has granted incentives to business in high technology industrial sectors locating in the Futian Free Trade Zone. Our intended pharmaceutical manufacture use qualifies for the tax incentives. Immtech Life Science is a Hong Kong company. E. Manufacturing 1. The Scientific Consortium Scientific Consortium members, specifically the combinatorial chemistry laboratory at Georgia State and the synthetic chemistry laboratory at UNC, have the capability to produce and inventory small quantities of the aromatic cations under license to us. To date, Georgia State and UNC have produced and supplied the dications requested in the quantities required under various testing agreements with third parties. We believe that Scientific Consortium members will continue to produce and deliver small quantities of compounds as needed for testing and commercialization purposes. 2. Third Party Sources On October 23, 2003, we entered into an agreement with Cardinal Health PTS, Inc. (Cardinal Health) to develop prototype formulations of DB289 to improve oral bioavailability DB289. Once the formulation is perfected by Cardinal Health we intend, to engage Cardinal Health to produce commercial quantities of good manufacturing practices ("GMP") grade with raw materials to be produced by another third party. Cardinal Health is the second largest producer of pharmaceuticals and other medical supplies in the United States. In February 2004, we entered into an agreement with Cambrex Charles City Inc. to improve the synthesis method for DB289, find methods to reduce the cost of manufacturing DB289, and to prepare the drug for production of commercial quantities of bulk GMP drug for clinical trials and sale. Cambrex is a global, diversified life sciences company dedicated to providing innovative products and services to accelerate drug discovery, development, and the manufacture of human therapeutics. 3. Our China Facility See disclosure above under the heading Immtech Life Science Limited. F. Strategy Our strategy is to develop oral drugs that are effective against infectious diseases and metabolic disorders by utilizing the aromatic cation/dicationic platform technology. Infectious diseases in the global population have increased significantly during the past 20 years and are the most common cause of death worldwide according to the WHO. Relatively few new drugs for treatment of infectious diseases have been brought to market during this period. New antibiotics are needed to overcome the problems of multi-drug resistance and the increasing number of new pathogens that are -17- causing diseases in the world. Metabolic disorders, including diabetes and cancer, cause illness and death world wide. Scientists have struggled for decades to find effective treatments for both diabetes and cancer. Our initial studies have demonstrated the dication platform to be effective to these two devastating metabolic disorders. We have been successful in developing a drug with a lower toxicity profile than Pentamidine that is orally available using our dication technology. We have leveraged our scientific partners and foundation funding while advancing our technology and human clinical trials in niche markets such as African sleeping sickness, as well as, in longer markets like malaria. We have advanced our pipeline in both antifungal and TB drugs, and established new programs in cancer, diabetes and neurological disorders. We plan to generate our first revenue by selling drugs into these niche markets with a U.S. FDA approval. We intend to proceed with the development and commercialization of aromatic cations/dications for drug products pursuant to our agreement with the Scientific Consortium as follows: o Generate revenues through the sales of human drug products to foundations in 2005; o Generate revenues by selling DB289 for compassionate use with an FDA approval; o Conclude Phase IIb pivotal trials of DB289 for treatment of malaria and prepare for Phase III pivotal trial; o Utilize the FDA's Fast-Track designation of DB289 for treatment of African sleeping sickness to expedite commercialization; o Generate shareholder value by developing our pipeline of prodrugs targeting TB, anti-fungal, diabetes and cancer; o Develop through our subsidiary Immtech HK a diabetes program with a financial partner; o Identify additional orally available dications to take into human clinical trials to further our fungal and TB programs; o Create joint ventures with pharmaceutical and biotechnology companies interested in developing oral products to treat diseases such as fungal, diabetes and cancer; o Develop joint ventures to advance our compounds as agents with Animal Health indications; and o Co-develop a pharmaceutical cancer program with a joint venture partner or a pharmaceutical company partner. -18- Our strategy is to commercialize aromatic cations/dications and generate revenues first in niche markets through selling drugs for diseases for which no other viable treatments exist and taking advantage of fast track FDA or corollary foreign approvals where permitted. We will continue to work with academic institutions and foundations to support our drug development programs. We seek to simultaneously develop treatments for infectious diseases, such as TB and fungal infections, and metabolic and neoplastic disorders like diabetes and cancer with substantial markets that afflict large populations of people. We believe our first product candidates demonstrate the power and versatility of the dication and Prodrug platform technologies. We believe our experience with these compounds in human clinical trials will help us expedite acceptance and obtain regulatory approval of our product candidates in other markets. We will continue to manage and oversee the programs and the results of research performed by members of the Scientific Consortium and to use business-sponsored research programs, government and foundation grants, strategic joint ventures and other forms of collaborative programs to advance product commercialization. We consider our current collaborative relationships significant to the successful development of our business. We believe that our collaborations will significantly minimize shareholder dilution while advancing drugs rapidly to commercialization. We plan to enter into additional arrangements in the future to develop, manufacture and market not only the product candidates on which we are currently focused, but also those dications which the Scientific Consortium members are developing for future commercialization. G. Research and Development Our current and future success will depend in large part on our ability to commercialize products based upon the platform technology for developing dications currently licensed to Immtech through the Consortium Agreement and future dications for which we have the exclusive worldwide rights to license from the Scientific Consortium. During the past three fiscal years, we estimate that we have spent approximately $581,000, $1,111,000 and $893,000, respectively, in fiscal years ended March 31, 2002, 2003 and 2004, on Company sponsored research and development and approximately $3,377,000, $1,459,000 and $2,400,000, respectively, in fiscal years ended March 31, 2002, 2003 and 2004, on research and development sponsored by others. All research and development activity for fiscal years ended March 31, 2002, 2003 and 2004 has been in support of our pharmaceutical commercialization effort. H. Patents and Licenses Our pharmaceutical compounds, including DB289 and DB075, are protected by multiple patents secured by members of the Scientific Consortium. We consider the protection of our proprietary technologies and products to be important to the success of our business and rely on a combination of patents, licenses, copyrights and trademarks to protect these technologies and products. To date, we have obtained exclusive licensing rights to 208 dication patents, 131 of which have been issued in the United States and in various global markets as of May 2004. In addition to the 181 -19- dication patents previously mentioned we own seven additional patents. Generally, U.S. patents have a term of 17 years from the date of issue for patents issued from applications submitted prior to June 8, 1995, and 20 years from the date of filing of the application in the case of patents issued from applications submitted on or after June 8, 1995. Patents in most other countries have a term of 20 years from the date of filing the patent application. 171 of our licensed patents, which includes 33 licensed U.S. patents, were submitted after June 8, 1995, including patents covering DB289, DB075 and our latest Prodrug formulation processes. Our policy is to file patent applications and defend the patents licensed to us covering the technology we consider important to our business in all countries where such protection is available and feasible. We intend to continue to file and defend patent applications we license or develop. Although we pursue and encourage patent protection and defend our patents and those licensed to us, obtaining patents for pharmaceutical drugs and their specific uses involves complex legal and factual questions and consequently involves a high degree of uncertainty. In addition, others may independently develop similar products, duplicate our potential products or design around the claims of any of our potential products. Because of the time delay in patent approval and the secrecy afforded the U.S. patent applications, we do not know if other applications, which might have priority over our applications, have been filed. We also rely on trade secrets, unpatented know-how and continuing technological innovation to develop and maintain our competitive position. Publication of discoveries in the scientific or patent literature tends to lag behind actual discoveries by at least several months. As a result, there can be no assurance that patents will be issued from any of our patent applications or from applications licensed to us. The scope of any of our issued patents may not be sufficiently broad to offer meaningful protection. In addition, our issued patents or patents licensed to us could be successfully challenged, invalidated or circumvented so that our patent rights would not create an effective competitive barrier. We also rely in part on trade secret, copyright and trademark protection of our intellectual property. We protect our trade secrets by entering into confidentiality agreements with third parties, employees and consultants. Employees and consultants sign agreements to assign to us their interests in patents and copyrights arising from their work for us. Key employees also agree not to engage in unfair competition with us after their employment by using our confidential information. We have additional secrecy measures as well. However, these agreements can be breached and, if they were, there might not be an adequate remedy available to us. Also, a third party could learn our trade secrets through means other than by breach of our confidentiality agreements, or our trade secrets could be independently developed by our competitors. 1. Patents Patents and patent applications for the chemical substance and use of pharmaceutical compounds to treat infections caused by PCP, TB, Cryptosporidium parvum, Giardia lamblia, Leishmania mexicana amazonesis, Trypanosoma brucei rhodesienes, various fungi, Plasmodium falciparum, HCV, BVDV and HIV have been -20- filed by the scientists of the Scientific Consortium members. We have exclusively licensed, or have the right to exclusively license, any of such patents for commercialization. We are obligated to reimburse or pay for patent protection of any such drugs that we license for commercialization. Patents and patent applications also protect certain processes for making Prodrugs and the uses of compounds to detect and treat specific diseases as well as a patent for a new method for making chemical compounds that form dimers when they are bound to DNA. Dimers are two identical chemical molecules that attach to a DNA's key site in series to cover a larger section (double) of a DNA's key site. On February 26, 2003, Scientific Consortium members were granted a patent by the U.S. Patent Office entitled "Prodrugs for Antimicrobial Amidines" for a proprietary technology to synthesize and manufacture Prodrugs. The patent protects a substantially advanced process for economically producing orally deliverable drugs. This newly patented process, licensed to Immtech under the Consortium Agreement, reduces the number of steps required to make dications orally available and thereby reduces the cost to manufacture Prodrug enhanced drugs. We are investigating the potential to sub-license this new Prodrug process to other drug manufacturers for use with their compounds designed to be taken orally and then activated in the blood stream. a. Patent Licenses --------------- Pursuant to the Consortium Agreement, licenses and options to license patents for the dications developed by the Scientific Consortium prior to January 15, 1997, which were previously licensed or optioned to Pharm-Eco, were transferred to us by Pharm-Eco as of March 2001. In accordance with the terms of the Consortium Agreement, we have obtained license rights to the patents covering the technology platform for making dicationic pharmaceutical drugs and to treat certain microbial infections with such products. To date, we have exclusively licensed 181 patents, which includes 51 U.S. patents. All of the patents on our dicationic product candidates have been filed by UNC jointly with the other academic institutions of the Scientific Consortium. b. Patent Rights ------------- Since January 1997, as required under the Consortium Agreement, we have filed, together with Scientific Consortium members, approximately 94 patent applications, of which approximately 34 have been granted. The Consortium Agreement grants us the right to license for commercialization product candidates underlying the patents and patent applications for dications produced by the Scientific Consortium. I. Governmental Regulation The development, manufacture and commercialization of drug products is subject to extensive regulation by both U.S. federal and, to a lesser extent, state governments and foreign governmental authorities in the areas in which our product -21- candidates are tested and manufactured, and in which potential products may be manufactured or sold. The Federal Food, Drug and Cosmetic Act ("FDCA") and other federal statutes and regulations govern or influence, among other things, the development, testing, manufacture, safety, labeling, storage, recordkeeping, approval, advertising, promotion, sale and distribution of pharmaceutical drugs. Pharmaceutical manufacturers are also subject to certain recordkeeping and reporting requirements, establishment registration and product listing, as well as FDA inspections. With respect to any non-biological "new drug" product with active ingredients not previously approved by the FDA, a prospective manufacturer must submit a full New Drug Application ("NDA"), including complete reports of pre-clinical, clinical and other studies, to prove the product's safety and efficacy. A full NDA may also need to be submitted for a drug product with a previously approved active ingredient if, among other things, the drug will be used to treat an indication for which the drug was not previously approved, or if the abbreviated procedure is otherwise not available. A manufacturer intending to conduct clinical trials in humans for a new drug may be required first to submit a Notice of Claimed Investigational Exception for an Investigational New Drug ("IND") to the FDA containing information relating to pre-clinical and clinical studies. INDs and full NDAs may be required to be filed to obtain approval of certain of our products, including those that do not qualify for abbreviated application procedures. The full NDA process, including clinical development and testing, is expensive and time consuming. Products being developed by us for sale in the United States may be regulated by the FDA as drugs or biologics. New drugs are subject to regulation under the FDCA, and biologics, in addition to being subject to certain provisions of the FDCA, are regulated under the Public Health Service Act. We believe that drug products developed by us or our collaborators will be regulated either as biologics or as new drugs. Both statutes and the regulations promulgated thereunder govern, among other things, the testing, manufacturing, safety, effectiveness, labeling, storage, record keeping, advertising and other promotional practices involving biologics or new drugs. FDA approval or other clearances must be obtained before clinical testing and before manufacturing and marketing of biologics and drugs. Obtaining FDA approval has historically been a costly and time consuming process. Generally, in order to gain FDA pre-market approval, a developer first must conduct pre-clinical studies in the laboratory and on animals to gain preliminary information on a drug candidate's effectiveness as well as identify any safety problems. The results of these studies are submitted as a part of an IND application, which the FDA must review before human clinical trials of a drug candidate can begin. The IND application includes a detailed description of the pre-clinical data and investigations to be undertaken. In order to commercialize any potential product, we or our collaborators must sponsor and file an IND and be responsible for initiating and overseeing clinical studies that demonstrate the safety and effectiveness necessary to obtain FDA approval. For Company or collaborator-sponsored INDs, the sponsor will be required to select -22- qualified investigators (usually physicians within medical institutions) to supervise the administration of the products and ensure that the investigations are conducted and monitored in accordance with FDA regulations, including the general investigational plan and protocols contained in the IND. Clinical trials are normally done in three phases, although the phases may overlap. Phase I trials are concerned primarily with the safety of the drug, involve fewer than 100 subjects and may take from six months to over one year to complete. Phase II trials normally involve a few hundred patients and are designed primarily to demonstrate effectiveness in treating or diagnosing the disease or condition for which the drug is intended, although short-term side-effects and risks in people whose health is impaired may also be examined. Phase III trials are expanded clinical trials with larger numbers of patients which are intended to evaluate the overall benefit-risk relationship of the drug and to gather additional information for proper dosage and labeling of the drug. In total, clinical trials generally take two to five years to complete, but may take longer. The FDA receives reports on the progress of each phase of clinical testing and the FDA may require the modification, suspension or termination of a clinical trial if it concludes that an unwarranted risk is presented to patients. If clinical trials of a new product are completed successfully, then the product sponsor may seek FDA marketing approval. If the product is regulated as a biologic, the FDA will require the submission and approval of both a Product License Application ("PLA") and an Establishment License Application ("ELA") before commercial marketing can commence. If the product is classified as a new drug, then the product sponsor must file an NDA with the FDA and receive approval before commencing commercial marketing. The NDA or PLA and ELA must include detailed information about the pharmaceutical drug or biologic and its manufacture and the results of product development, pre-clinical studies and clinical trials. The testing and approval processes require substantial time and effort and there can be no assurance that any approval will be granted on a timely basis, if at all. NDAs and PLAs submitted to the FDA can take, on average, two to five years to receive approval. If questions arise during the FDA review process, then approval can take more than five years. Notwithstanding the submission of relevant data, the FDA may ultimately decide that the NDA or PLA does not satisfy the FDA's regulatory criteria for approval and deny approval or require additional clinical studies. In addition, the FDA may condition marketing approval on the conduct of specific post-marketing studies to further evaluate safety and effectiveness. Even if FDA regulatory clearances are obtained, a marketed product is always subject to continual review and later discovery of previously unknown problems or failure to comply with the applicable regulatory requirements may result in restrictions on the marketing of a product or withdrawal of the product from the market, as well as possible civil or criminal sanctions. The Drug Price Competition and Patent Restoration Act of 1984, known as the Waxman-Hatch Act, established abbreviated NDA ("ANDA") procedures for obtaining FDA approval for generic versions of many non-biological drugs for which patent or marketing exclusivity rights have expired and which are bioequivalent to previously approved drugs. "Bioequivalence" for this purpose, with certain exceptions, generally means that the proposed generic formulation is absorbed by the body at the same rate and extent as a previously approved "reference drug." Approval to -23- manufacture these drugs is obtained by filing abbreviated applications, such as ANDAs. As a substitute for clinical studies, the FDA requires data indicating the ANDA drug formulation is bio-equivalent to the previously approved reference drug. The advantage of the ANDA approval mechanism, compared to an NDA, is that an ANDA applicant is not required to conduct pre-clinical and clinical studies to demonstrate that the product is safe and effective for its intended use and may rely, instead, on studies demonstrating bioequivalence to a previously approved reference drug. In addition to establishing ANDA approval mechanisms, the Waxman-Hatch Act fosters pharmaceutical innovation through such incentives as non-patent exclusivity and patent restoration. This Act provides two distinct exclusivity provisions that either preclude the submission or delay the approval of an ANDA. A five-year exclusivity period is provided for new chemical compounds and a three-year marketing exclusivity period is provided for changes to previously approved drugs that are based on new clinical investigations essential to the approval. The three-year marketing exclusivity period may be applicable to the approval of a novel drug delivery system. The marketing exclusivity provisions apply equally to patented and non-patented drug products. These provisions do not delay or otherwise affect the approvability of full NDAs even when effective ANDA approvals are not available. For drugs covered by patents, patent extension may be provided for up to five years as compensation for reduction of the effective life of the patent resulting from time spent in conducting clinical trials and in FDA review of a drug application. In addition to obtaining pre-market approval for certain of our products, we will be required to maintain all facilities that produce our product candidates for commercial consumption in the United States in compliance with the FDA's current Good Manufacturing Practice ("cGMP") requirements. In addition to compliance with cGMP, each pharmaceutical manufacturer's facilities must be registered with the FDA. Manufacturers must also be registered with the Drug Enforcement Agency, or DEA, and similar state and local regulatory authorities if they handle controlled substances, and with the Environmental Protection Agency, or EPA, and similar state and local regulatory authorities if they generate toxic or dangerous wastes. Noncompliance with applicable requirements can result in fines, recall or seizure of products, total or partial suspension of production and distribution, refusal of the government to enter into supply contracts or to approve NDAs, ANDAs or other applications and criminal prosecution. The FDA also has the authority to revoke for cause drug approvals previously granted. For international markets, a pharmaceutical company is subject to regulatory requirements, inspections and product approvals substantially the same as those in the United States. In connection with any future marketing, distribution and license agreements that we may enter, our licensees may accept or assume responsibility for such foreign regulatory approvals. The time and cost required to obtain these international market approvals may be greater or lesser than those required for FDA approval. Product development and approval within this regulatory framework takes a number of years, involves the expenditure of substantial resources and is uncertain. -24- Many drug products ultimately do not reach the market because they are not found to be safe or effective or cannot meet the FDA's other regulatory requirements. In addition, the current regulatory framework may change and additional regulations may arise at any stage of our product development that may affect approval, delay the submission or review of an application or require additional expenditures by us. We may not be able to obtain necessary regulatory clearances or approvals on a timely basis, if at all, for any of our products under development, and delays in receipt or failure to receive such clearances or approvals, the loss of previously received clearances or approvals or failure to comply with existing or future regulatory requirements could have a material adverse effect on our business. J. Competition Competition in the pharmaceutical and biotechnology industries is intense. Factors such as scientific and technological developments, the procurement of patents, timely governmental approval for testing, manufacturing and marketing, availability of funds, the ability to commercialize product candidates in an expedient fashion and the ability to obtain governmental approval for testing, manufacturing and marketing play a significant role in determining our ability to effectively compete. Furthermore, our industry is subject to rapidly evolving technology that could result in the obsolescence of any product candidates prior to profitability. Our competitors may have substantially greater financial, technical and human resources than we have and may be better equipped to develop, manufacture and market products. Many of our competitors have concentrated their efforts in the development of human therapeutics and developed or acquired internal biotechnology capabilities. We have utilized the Scientific Consortium as our research and development arm. In addition, many of these companies have extensive experience in pre-clinical testing and human clinical trials and in obtaining regulatory approvals. Our competitors may succeed in obtaining approval for products more rapidly than us and in developing and commercializing products that are safer and more effective than those that we propose to develop. Competitors, as well as academic institutions, governmental agencies and private research organizations, also compete with us in acquiring rights to products or technologies from universities, and recruiting and retaining highly qualified scientific personnel and consultants. The timing of market introduction of our potential products or of competitors' products will be an important competitive factor. Accordingly, the relative speed with which we can develop products, complete pre-clinical testing, human clinical trials and regulatory approval processes and supply commercial quantities to market will influence our ability to bring a product to market. Our competition will be determined in part by the potential indications for which our products are developed and ultimately approved by regulatory authorities. We rely on our collaborations with the Scientific Consortium members and other joint venture partners to enhance our competitive edge by providing manufacturing, testing and commercialization support. Currently, DB289 is in clinical trials to treat African sleeping sickness, PCP, and malaria. Other drugs moving forward in our pipeline address -25- markets for new drugs for use in treating fungal, TB, and diabetic diseases. The following table lists major competitors and their drugs by disease: ------------------------------------------------------------------------------------------------------------------------------ African sleeping Malaria PCP sickness Antifungals TB ------------------------------------------------------------------------------------------------------------------------------ o Quinine o Bactrim o Pentamidine o Fluconazole Rifampin (Watson (Hoffman (Aventis) (Pfizer) (Aventis, Pharma.) LaRoche) Ciba Geneva) ------------------------------------------------------------------------------------------------------------------------------ o Chloroquine o Pentamidine o Melarsoprol o Itraconazole o Isoniazid (Sanofi-Synthelabo (Aventis) (Aventis) o Ketoconazole (Lannett Co. Inc.) o Miconazole Inc., (Johnson & Bristol-Meyers Johnson) Squibb, Hoffman LaRoche) ------------------------------------------------------------------------------------------------------------------------------ o Mefloquine o Eflornithine o Terbinafine o Pyrazinamide (Hoffman (Aventis) (Novartis) (Lederle LaRoche) Laboratories, ICN Canada Pharmaceuticals, Pharmascience Inc.) ------------------------------------------------------------------------------------------------------------------------------ o Amodiaquine o Suramin o Caspofungin o Ethambutol (Pfizer) (Bayer) (Merck) (Lederle Laboratories, ICN Canada Pharmaceuticals) ------------------------------------------------------------------------------------------------------------------------------ o Amphotericin B lipid complex (Fujisawa) ------------------------------------------------------------------------------------------------------------------------------ We are developing products to treat infectious diseases and metabolic disorders. Our drug development program closest to commercialization, is for the treatment of African sleeping sickness, has been funded in large part by a grant to a scientific consortium lead by UNC from The Gates Foundation. The Gates Foundation has chosen to support the African sleeping sickness program because there currently exists no effective treatment for the disease. We believe The Gates Foundation has financed this project because the likelihood that a major pharmaceutical company would develop a treatment for the disease is small because treatments for diseases that affect economically-challenged populations, without charitable assistance, are less profitable than treatments for diseases that affect more developed nations. Our efforts to develop aromatic dicationic Prodrugs for treatment of African sleeping sickness contributes greatly to validating and advancing our technology platform and establishing pharmacological safety and dosage criteria for future compounds aimed at more mainstream markets. We have listed in the table above, where applicable, current treatments and the names of the manufacturers of those products used to treat disease for which we are developing product candidates, however, each of the products listed has limitations in terms of effectiveness -26- to treat the disease, toxicity, severity of side effects, and/or difficulty of delivery (for example, Pentamidine must be administered either intravenously or by inhalation. We therefore believe that competition for our product candidates for certain indications has yet to be developed or approved. EMPLOYEES We currently have 11 employees, five of whom hold advanced degrees. Five work in support of clinical trials, research and development and regulatory compliance, while six work in general and administrative capacities which includes business development, investor relations, finance and administration. Through our agreement with the Scientific Consortium, approximately 55 scientists are engaged in the research and development of the dications. We expect to add new employees in our regulatory and clinical development departments as our programs advance. RISK FACTORS There is no assurance that we will successfully develop a commercially viable product; our most advanced product candidate is in Phase II human clinical trials. We are at an early stage of human clinical trials, and in some cases pre-clinical, development activities required for drug approval and commercialization. Since our formation in October 1984, we have engaged in research and development programs, expanding our network of scientists and scientific advisors, licensing technology agreements and advancing the commercialization of the dication technology platform. We have generated no revenue from product sales, do not have any products currently available for sale, and none are expected to be commercially available for sale until after March 31, 2005, if at all. There can be no assurance that the research we fund and manage will lead to commercially viable products. Our most advanced programs are in the Phase II human clinical testing stage using our first compound DB289 for several indications including trypanosomiasis (African sleeping sickness), PCP pneumonia, and malaria and must undergo substantial additional regulatory review prior to commercialization. We have a history of losses and an accumulated deficit; our future profitability is uncertain. We have experienced significant operating losses since our inception and we expect to incur additional operating losses as we continue research and development, clinical trial and commercialization efforts. As of March 31, 2004, we had an accumulated deficit of approximately $58,539,000. Losses from operations were approximately $4,693,000 and $12,866,000, for the fiscal years ended March 31, 2003 and March 31, 2004, respectively. We will need substantial additional funds in future years to continue our research and development; if financing is not available, we may be required to reduce spending for our research programs, cease operations or pursue other financing alternatives. Our operations to date have consumed substantial amounts of cash. Negative cash flow from operations is expected to continue in the foreseeable future. Without substantial additional financing, we may be required to reduce some or all of our research programs or cease operations. Our cash requirements may vary materially from those now planned because of results of research and development, results of pre-clinical and clinical testing, responses to our grant requests, relationships with strategic partners, changes in the focus and direction of our research and development programs, competitive and technological advances, the FDA and foreign regulatory process and other factors. In any of these circumstances, we may require substantially more funds than we currently have available or currently intend to raise to continue our business. We may seek to satisfy future funding requirements through public or private -27- offerings of equity securities, by collaborative or other arrangements with pharmaceutical or biotechnology companies, issuance of debt or from other sources. Additional financing may not be available when needed or may not be available on acceptable terms. If adequate financing is not available, we may not be able to continue as a going concern or may be required to delay, scale back or eliminate certain research and development programs, relinquish rights to certain technologies or product candidates, forego desired opportunities or license third parties to commercialize our products or technologies that we would otherwise seek to develop internally. To the extent we raise additional capital by issuing equity securities, ownership dilution to existing stockholders will result. We receive funding primarily from technology licensing, grants, research and development programs and from sales of our equity securities. To date we have directed most of such funds not used for general and administrative overhead toward our research and development and commercialization programs (including preparation of submissions to regulatory agencies for product licensing). Until one or more of our product candidates is approved for sale, our funding is limited to funds received from testing and research agreements, licensing of our technology and potential fees associated with interim leasing of our properties while we develop them for product manufacture. We do not have employment contracts with any employees other than our CEO, T. Stephen Thompson. We have an employment agreement with our CEO, T. Stephen Thompson that renews annually in April of each year unless 30 day prior notice of non-renewal is given by either party to the other. Mr. Thompson renewed his employment with us this year and has not expressed any indication that he desires to leave our employ or retire. All of our other employees are "at will" and may leave at any time, however, none have as of this date, expressed any intention to do so. We do not have "key-man" life insurance policies on any of our executives, including Mr. Thompson. Most of our business' financial aspects, including investor relations, intellectual property control and corporate governance, are under the direct supervision of Cecilia Chan and Gary Parks. Together with Mr. Thompson, Ms. Chan and Mr. Parks hold institutional knowledge and business savvy that they utilize to assist us to forge new relationships and exploit new business opportunities without diminishing or undermining existing programs and obligations. Neither Ms. Chan nor Mr. Parks have employment contracts with us, however, neither has indicated any intention to retire or leave our employ. Some of our proprietary intellectual property is developed by scientists that are not employed by us. Our business depends to a significant degree on the continuing contributions of our key management, scientific and technical personnel, as well as on the continued discoveries of scientists, researchers and specialists at The University of North Carolina at Chapel Hill, Georgia State, Duke University and Auburn University (collectively, the "Scientific Consortium") and other research groups that assist in the development of our product candidates. Substantial amounts of our proprietary intellectual property is developed by scientists who are -28- employed by the universities that comprise the Scientific Consortium and other research groups. We do not have control over, knowledge of, or access to those employment arrangements. We have not been advised by any of the key members of our company, the scientific research groups or of the Scientific Consortium of their intention to leave their employ or the program. There can be no assurance that the loss of certain members of management or the scientists, researchers and technicians from the Scientific Consortium universities would not materially adversely affect our business. Additional research grants needed to fund our operations may not be available or, if available, not on terms acceptable to us. We have funded our product development and operations as of March 31, 2004 through a combination of sales of equity instruments and revenue generated from research agreements and grants. As of March 31, 2004, our accumulated deficit was approximately $58,539,000 of which approximately $11,259,000 was funded either directly or indirectly with grant funds and payments from research and testing agreements. In March 2001 we entered into a clinical research subcontract with UNC, funded by a $15.1 million grant from The Gates Foundation to UNC for the study of African sleeping sickness and leishmaniasis, under which UNC is to pay to us $9.8 million in installments over a period not to exceed five years based on our achieving certain milestones. We entered into a second subcontract with UNC under which we are to receive over $2.4 million based on a separate $2.7 million grant from the Gates Foundation to UNC to accelerate the African sleeping sickness study. In November 2003, we entered into a Testing Agreement with Medicines For Malaria Venture, a foundation established in Switzerland ("MMV") and UNC, pursuant to which we, with the support of MMV and UNC, are conducting a proof of concept study of DB289, including Phase II and Phase III human clinical trials, and will pursue drug development activities of DB289 alone, or in combination with other anti-malarial drugs, with the goal of obtaining marketing approval of a product for the treatment of malaria. Under the terms of the agreement, MMV has advanced to us $668,000 for human clinical trials and has committed to fund additional budgeted amounts, subject to attainment of certain milestones, for additional clinical trials and regulatory preparation and filing costs for the approval to market DB289 for treatment of malaria by at least one internationally accepted regulatory body and one malaria endemic country. We forecast such costs to be approximately $8.2 million over the next three years. We will continue to apply for new grants to support continuing research and development of our dication platform technology and other product candidates. The process of obtaining grants is extremely competitive and there can be no assurance that any of our grant applications will be acted upon favorably. Some charitable organizations may request licenses to our proprietary information or may impose price restrictions on the products we develop with grant funds. We may not be able to negotiate terms that are acceptable to us with such organizations. In the event we are unable to raise sufficient funds to advance our product developments with grant funds we may seek to raise additional capital with the issuance of debt -29- or equity securities. There can be no assurance that we will be able to place or sell debt or equity securities on terms acceptable to us and, if we sell equity, existing stockholders will suffer dilution (see Risk Factors, this section, entitled "Shares eligible for future sale may adversely affect our ability to sell equity securities," and "Our outstanding options and warrants may adversely affect our ability to consummate future equity financings due to the dilution potential to future investors"). None of our product candidates have been approved for sale by any regulatory agency; approval is required before we can sell drug products commercially. All of our product candidates, including DB289 and DB075, require additional clinical testing, regulatory approval and development of marketing and distribution channels, all of which are expected to require substantial additional investment prior to commercialization. There can be no assurance that any of our product candidates will be successfully developed, prove to be safe and effective in human clinical trials, meet applicable regulatory standards, be capable of being produced in commercial quantities at acceptable costs, be eligible for third party reimbursement from governmental or private insurers, be successfully marketed or achieve market acceptance. If we are unable to commercialize our product candidates in a timely manner we may be required to seek additional funding, reduce or cancel some or all of our development programs, sell or license some of our proprietary information or cease operations. There are substantial uncertainties related to clinical trials that may result in the extension, modification or termination of one or more of our programs. In order to obtain required regulatory approvals for the commercial sale of our product candidates, we must demonstrate through human clinical trials that our product candidates are safe and effective for their intended uses. Prior to conducting human clinical trials we must obtain governmental approvals from the host nation, approval from the U.S. to export our product candidate to the test site and qualify a sufficient number of volunteer patients that meet our trial criteria. If we do not obtain required governmental consents or if we do not enroll a sufficient number of patients in a timely manner or at all, our trial expenses could increase, results may be delayed or the trial may be cancelled. We may find, at any stage of our research and development, that product candidates that appeared promising in earlier clinical trials do not demonstrate safety or effectiveness in later clinical trials and therefore do not receive regulatory approvals. Despite the positive results of our pre-clinical testing and human clinical trials those results may not be predictive of the results of later clinical trials and large-scale testing. Companies in the pharmaceutical and biotechnology industries have suffered significant setbacks in various stages of clinical trials, even after promising results had been obtained in early-stage human clinical trials. Completion of human clinical trials may be delayed by many factors, including slower than anticipated patient enrollment, difficulty in securing sufficient supplies of clinical trial materials or adverse events occurring during clinical trials. For instance, once we obtain permission to run a human trial, there are strict criteria regulating who we can test. In the case of African sleeping sickness, we are subject to civil unrest in sub-Sahara Africa where local rebels -30- could close clinics and dramatically reduce enrollment rates, and make it difficult to conduct trials. In another case, our PCP-trial could encounter difficulties in finding potential patients because our initial regimen requires patients to first fail other treatment programs in order to be eligible for our treatment. Completion of testing, studies and trials may take several years, and the length of time varies substantially with the type, complexity, novelty and intended use of the product. Delays or rejections may be based upon many factors, including changes in regulatory policy during the period of product development. No assurance can be given that any of our development programs will be successfully completed, that any Investigational New Drug ("IND") application filed with the FDA (or any foreign equivalent filed with the appropriate foreign authorities) will become effective, that additional clinical trials will be allowed by the FDA or other regulatory authorities, or that clinical trials will commence as planned. There have been delays in our testing and development schedules due to the aforementioned conditions and funding and patient enrollment difficulties and there can be no assurance that our future testing and development schedules will be met. We do not currently have pharmaceutical manufacturing capability, which could impair our ability to develop commercially viable products at reasonable costs. Our ability to commercialize product candidates will depend in part upon our ability to have manufactured or develop manufacturing capability to manufacture our product candidates, either directly or through third parties, at a competitive cost and in accordance with FDA and other regulatory requirements. We currently lack facilities and personnel to manufacture our product candidates. There can be no assurance that we will be able to acquire such resources, either directly or through third parties, at reasonable costs, if we develop commercially viable products. We have acquired a facility in which we intend to commence construction of a pharmaceutical manufacturing plant in the PRC with our subsidiary Immtech Hong Kong Limited. Operation of such a facility is subject to various governmental approvals, which may be difficult or impossible to obtain. There can be no guarantee that products manufactured at this facility will be accepted in all countries where we desire to sell our future products. We are dependent on third-party relationships for critical aspects of our business; problems that develop in these relationships may increase costs and/or diminish our ability to develop our product candidates. We use the expertise and resources of strategic partners and third parties in a number of key areas, including (i) research and development, (ii) pre-clinical and human clinical trials and (iii) manufacture of pharmaceutical drugs. We have licensing and exclusive commercialization rights to a dicationic pharmaceutical platform and are developing drugs intended for commercial use based on that platform. This strategy creates risks by placing critical aspects of our business in the hands of third parties, whom we may not be able to control. If these third parties do not perform in a timely and satisfactory manner, we may incur costs and delays as we seek alternate sources of such products and services, if available. Such costs and -31- delays may have a material adverse effect on our business if the delays jeopardize our licensing arrangements by causing us to become non-compliant with certain license agreements. We may seek additional third-party relationships in certain areas, particularly in clinical testing, marketing, manufacturing and other areas where pharmaceutical and biotechnology company collaborators will enable us to develop particular products or geographic markets that are otherwise beyond our current resources and/or capabilities. There is no assurance that we will be able to obtain any such collaboration or any other research and development, manufacturing or clinical trial arrangements. Our inability to obtain and maintain satisfactory relationships with third parties may have a material adverse effect on our business by slowing our ability to develop new products, requiring us to expand our internal capabilities, increasing our overhead and expenses, hampering future growth opportunities or causing us to delay or terminate affected programs. We are uncertain about the ability to protect or obtain necessary patents and protect our proprietary information; our ability to develop and commercialize our product candidates would be compromised without adequate intellectual property protection. We have spent and continue to spend considerable funds to develop our product candidates and we are relying on the potential to exploit commercially without competition the results of our product development. Much of our intellectual property is licensed to us under various agreements including the Consortium Agreement. It is the primary responsibility of the discoverer to develop his, her or its invention confidentially, insure that the invention is unique, and to obtain patent protection. In most cases, our role is to reimburse patent related costs after we decide to develop any such invention. We therefore rely on the inventors to insure that technology licensed to us is adequately protected. Without adequate protection for our intellectual property we believe our ability to realize profits on our future commercialized product would be diminished. Without protection, competitors might be able to copy our work and compete with our products without having invested in the development. There can be no assurance that any particular patent will be granted or that issued patents will provide us, directly or through licenses, with the intellectual property protection contemplated. Patents and licenses of patents can be challenged, invalidated or circumvented. It is also possible that competitors will develop similar products simultaneously. Our breach of any license agreement or the failure to obtain a license to any technology or process which may be required to develop or commercialize one or more of our product candidates may have a material adverse effect on our business including the need for additional capital to develop alternate technology, the potential that competitors may gain unfair advantage and lessen our expectation of potential future revenues. The pharmaceutical and biotechnology fields are characterized by a large number of patent filings, and a substantial number of patents have already been issued to other pharmaceutical and biotechnology companies. Third parties may have filed applications for, or may have been issued, certain patents and may obtain additional patents and proprietary rights related to products or processes competitive with or similar to those that we are attempting to develop and commercialize. We may not be aware of all of the patents potentially adverse to our interests that may have been issued to others. No assurance can be given that patents do not -32- exist, have not been filed or could not be filed or issued, which contain claims relating to or competitive with our technology, product candidates, product uses or processes. If patents have been or are issued to others containing preclusive or conflicting claims, then we may be required to obtain licenses to one or more of such patents or to develop or obtain alternative technology. There can be no assurance that the licenses or alternative technology that might be required for such alternative processes or products would be available on commercially acceptable terms, or at all. Because of the substantial length of time and expense associated with bringing new drug products to market through the development and regulatory approval process, the pharmaceutical and biotechnology industries place considerable importance on patent and trade secret protection for new technologies, products and processes. Since patent applications in the United States are confidential until patents are issued and since publication of discoveries in the scientific or patent literature often lag behind actual discoveries, we cannot be certain that we (or our licensors) were the first to make the inventions covered by pending patent applications or that we (or our licensors) were the first to file patent applications for such inventions. The patent positions of pharmaceutical and biotechnology companies can be highly uncertain and involve complex legal and factual questions and, therefore, the breadth of claims allowed in pharmaceutical and biotechnology patents, or their enforceability, cannot be predicted. There can be no assurance that any patents under pending patent applications or any further patent applications will be issued. Furthermore, there can be no assurance that the scope of any patent protection will exclude competitors or provide us competitive advantages, that any of our (or our licensors') patents that have been issued or may be issued will be held valid if subsequently challenged, or that others, including competitors or current or former employers of our employees, advisors and consultants, will not claim rights in, or ownership to, our (or our licensors') patents and other proprietary rights. There can be no assurance that others will not independently develop substantially equivalent proprietary information or otherwise obtain access to our proprietary information, or that others may not be issued patents that may require us to obtain a license for, and pay significant fees or royalties for, such proprietary information. We rely on technology developed by others and shared with collaborators to develop our product candidates which puts our proprietary information at risk of unauthorized disclosure. We rely on trade secrets, know-how and technological advancement to maintain our competitive position. Although we use confidentiality agreements and employee proprietary information and invention assignment agreements to protect our trade secrets and other unpatented know-how, these agreements may be breached by the other party thereto or may otherwise be of limited effectiveness or enforceability. We are licensed to commercialize technology from a dication platform developed by a Scientific Consortium, comprised primarily of scientists employed by universities in an academic setting. The academic world is improved by the sharing of information. As a business, however, the sharing of information whether through publication of research, academic lectures or general intellectual discourse among contemporaries is not conducive to protection of proprietary information. Our proprietary information may fall into the possession of unintended parties without our knowledge through customary academic information sharing. -33- At times we may enter into confidentiality agreements with other companies, allowing them to test our technology for potential future licensing, in return for milestone and royalty payments should any discoveries result from the use of our proprietary information. We cannot be assured that such parties will honor these confidentiality agreements subjecting our intellectual property to unintended disclosure. The pharmaceutical and biotechnology industries have experienced extensive litigation regarding patent and other intellectual property rights. We could incur substantial costs in defending suits that may be brought against us (or our licensors) claiming infringement of the rights of others or in asserting our (or our licensors') patent rights in a suit against another party. We may also be required to participate in interference proceedings declared by the U.S. Patent and Trademark Office or similar foreign agency for the purpose of determining the priority of inventions in connection with our (or our licensors') patent applications. Adverse determinations in litigation or interference proceedings could require us to seek licenses (which may not be available on commercially reasonable terms) or subject us to significant liabilities to third parties, and could therefore have a material adverse effect on our business by increasing our expenses and having an adverse effect on our business. Even if we prevail in an interference proceeding or a lawsuit, substantial resources, including the time and attention of our officers, would be required. Confidentiality agreements may not adequately protect our intellectual property which could result in unauthorized disclosure or use of our proprietary information. We require our employees, consultants and third-parties with whom we share proprietary information to execute confidentiality agreements upon the commencement of their relationship with us. The agreements generally provide that trade secrets and all inventions conceived by the individual and all confidential information developed or made known to the individual during the term of the relationship will be our exclusive property and will be kept confidential and not disclosed to third parties except in specified circumstances. There can be no assurance, however, that these agreements will provide meaningful protection for our proprietary information in the event of unauthorized use or disclosure of such information. If our unpatented proprietary information is publicly disclosed before we have been granted patent protection, our competitors could be unjustly enriched and we could lose the ability to profitably develop products from such information. Our industry has significant competition; our product candidates may become obsolete prior to commercialization due to alternative technologies thereby rendering our development efforts obsolete or non-competitive. The pharmaceutical and biotechnology fields are characterized by extensive research efforts and rapid technological progress. Competition from other pharmaceutical and biotechnology companies and research and academic institutions is intense and other companies are engaged in research and product development for treatment of the same diseases that we target. New developments in pharmaceutical and biotechnology fields are expected to continue at a rapid pace in both industry and academia. There can be no assurance that research and -34- discoveries by others will not render some or all of our programs or products non-competitive or obsolete. We are aware of other companies and institutions dedicated to the development of therapeutics similar to those we are developing, including Aventis Pharmaceuticals, Inc., Hoffman-LaRoche Ltd., Sanofi-Synthelabo Inc., Pfizer Inc., and Bayer Corporation. Many of our existing or potential competitors have substantially greater financial and technical resources than we do and therefore may be in a better position to develop, manufacture and market pharmaceutical products. Many of these competitors are also more experienced performing pre-clinical testing and human clinical trials and obtaining regulatory approvals. The current or future existence of competitive products may also adversely affect the marketability of our product candidates. In the event some or all of our programs are rendered non-competitive or obsolete, we do not currently have alternative strategies to develop new product lines or financial resources to pursue such a course of action. There is no assurance that we will receive FDA or corollary foreign approval for any of our product candidates for any indication; we are subject to government regulation for the commercialization of our product candidates. We have not made application to the U.S. FDA or any other regulatory agency to sell commercially or label any of our product candidates. We or our test collaborators have received licenses from the FDA to export DB289 for testing purposes and have been approved to conduct human clinical trials for various indications in each of the Democratic Republic of Congo, Angola, Thailand and Peru. All new pharmaceutical drugs and biologics, including our product candidates, are subject to extensive and rigorous regulation by the federal government, principally the FDA under the Federal Food, Drug and Cosmetic Act ("FDCA") and other laws including, in the case of biologics, the Public Health Services Act, and by state, local and foreign governments. Such regulations govern, among other things, the development, testing, manufacture, labeling, storage, pre-market clearance or approval, advertising, promotion, sale and distribution of pharmaceutical drugs and biologics. If drug products or biologics are marketed abroad, they are subject to extensive regulation by foreign governments. Failure to comply with applicable regulatory requirements may subject us to administrative or judicially imposed sanctions such as civil penalties, criminal prosecution, injunctions, product seizure or detention, product recalls, total or partial suspension of production and FDA refusal to approve pending applications. Each of our product candidates must be approved for each indication for which we believe it to be viable. We have not yet determined from which regulatory bodies we will seek approval for our product candidates or for which indications. Once determined, the approval process is subject to those agencies' policies and acceptance of those agencies' approvals, if obtained, in the countries where we intend to market our product candidates. -35- We have not received regulatory approval in the United States or any foreign jurisdiction for the commercial sale of any of our product candidates. On April 23, 2004 the FDA granted fast-track designation for DB289, our first oral drug, for treatment of African sleeping sickness (trypanosomiasis), meaning the FDA will accept initial late-stage data from us rather than waiting for the entire Phase III clinical trial data to be submitted together for consideration of approval to market the drug. The process of obtaining FDA and other required regulatory approvals, including foreign approvals, often takes many years and varies substantially based upon the type, complexity and novelty of the products involved and the indications being studied. Furthermore, the approval process is extremely expensive and uncertain. There can be no assurance that our product candidates will be approved for commercial sale in the United States by the FDA or regulatory agencies in foreign countries. The regulatory review process can take many years and we will need to raise additional funds to complete the regulatory review process for our current product candidates. Therefore, the failure to receive FDA approval would have a material adverse effect on our business by precluding us from marketing and selling such products in the United States and preventing us from representing to other nations that the U.S. FDA has approved our products to facilitate accelerated review procedures in those nations and therefore negatively impacting our ability to generate future revenues. Even if regulatory approval of a product is granted, there can be no assurance that we will be able to obtain the labeling claims (a labeling claim is a product's description and its FDA permitted uses) necessary or desirable for the promotion of such product. FDA regulations prohibit the marketing or promotion of a drug for unapproved indications. Furthermore, regulatory marketing approval may entail ongoing requirements for post-marketing studies if regulatory approval is obtained; we will then be subject to ongoing FDA obligations and continued regulatory review. In particular, we, or our third party manufacturers, will be required to adhere to Good Manufacturing Practices ("GMP"), which require us (or our third party manufacturers) to manufacture products and maintain records in a prescribed manner with respect to manufacturing, testing and quality control. Further, we (or our third party manufacturers) must pass a manufacturing facilities pre-approval inspection by the FDA or corollary agency before obtaining marketing approval. Failure to comply with applicable regulatory requirements may result in penalties, such as restrictions on a product's marketing or withdrawal of the product from the market. In addition, identification of certain side effects after a drug is on the market or the occurrence of manufacturing problems could cause subsequent withdrawal of approval, reformulation of the drug, additional pre-clinical testing or clinical trials and changes in labeling of the product. Prior to the submission of an application for FDA approval, our pharmaceutical drugs and biologics undergo rigorous pre-clinical and clinical testing, which may take several years and the expenditure of substantial financial and other resources. Before commencing clinical trials in humans in the United States, we must submit to the FDA and receive clearance of an IND. There can be no assurance that submission of an IND for future clinical testing of any of our product candidates under development or other future product candidates would result in FDA permission to commence clinical trials or that we will be able to obtain the necessary approvals for future clinical testing in any foreign jurisdiction. Further, there can be no assurance that if such testing of product candidates under development is completed, any such drug compounds will be accepted for formal review by the FDA or any foreign regulatory body -36- or approved by the FDA for marketing in the United States or by any such foreign regulatory bodies for marketing in foreign jurisdictions. If a product is regulated as a biologic, the FDA will require the submission and approval of both a Product License Application ("PLA") and an Establishment License Application ("ELA") before commercial marketing can commence. The PLA must include detailed information about the biologic, its manufacture and the results of product development, pre-clinical studies and clinical trials. The FDA's time to review PLAs and ELAs averages two to five years. The FDA may ultimately decide that the PLA and ELA do not satisfy the regulatory criteria for approval and deny approval or require additional clinical studies. Future federal, state, local or foreign legislation or administrative acts could also prevent or delay regulatory approval of our pharmaceutical drug and biologic candidates. We anticipate filing a NDA with the FDA for compassionate use of DB289 as a treatment for trypanosomiasis in sub-Sahara Africa in calendar year 2005. Our most advanced programs are developing products intended for sale in countries that may not have established pharmaceutical regulatory agencies. Some of the intended markets for our treatment of African sleeping sickness and malaria are in countries without developed pharmaceutical regulatory agencies. We plan in such cases to try first to obtain regulatory approval from a recognized pharmaceutical regulatory agency such as the U.S. FDA or one or more European agencies and then to apply to the targeted country for recognition of the foreign approval. Because the countries where we intend to market treatments for African sleeping sickness and malaria are not obligated to accept foreign regulatory approvals and because those countries do not have standards of their own for us to rely upon, we may be required to provide additional documentation or complete additional testing prior to distributing our products in those countries. There is uncertainty regarding the availability of health care reimbursement for purchasers of our anticipated products; health care reform may negatively impact the ability of prospective purchasers of our anticipated products to pay for such products. Our ability to commercialize any of our product candidates will depend in part on the extent to which reimbursement for the costs of the resulting drug or biologic will be available from government health administration authorities, private health insurers, charities and others. Many of our product candidates, including treatments for trypanosomiasis, malaria and tuberculosis, would be in the greatest demand in developing nations, many of which do not maintain comprehensive health care systems with the financial resources to pay for such drugs. We do not know to what extent governments, private charities, international organizations and others would contribute toward bringing newly developed drugs to developing nations. Even among drugs sold in developed countries, significant uncertainty exists as to the reimbursement status of newly approved health care products. There can be no assurance of the availability of third-party insurance reimbursement coverage enabling us to establish and maintain price levels sufficient for realization of a profit on our investment in developing pharmaceutical drugs and biologics. Government and other third-party payers are increasingly attempting to contain health care costs by limiting both coverage and the level of reimbursement for new drug or biologic products approved for marketing by the FDA and by refusing, in some cases, to provide any -37- coverage for uses of approved products for disease indications for which the FDA has not granted marketing approval. If adequate coverage and reimbursement levels are not provided by government and third-party payers for uses of our anticipated products, the market acceptance of these products would be adversely affected. Health care reform proposals are continually introduced in the United States Congress and in various state legislatures and there is no guarantee that such proposals will not be introduced in the future. We cannot predict when any proposed reforms will be implemented, if ever, or the effect of any implemented reforms on our business. Implemented reforms may have a material adverse effect on our business by reducing or eliminating the availability of third-party reimbursement for our anticipated products or by limiting price levels at which we are able to sell such products. If reimbursement is not available for our products, health care providers may prescribe alternative remedies if available. Patients, if they cannot afford our products, may do without. In addition, if we are able to commercialize products in overseas markets, then our ability to achieve success in such markets may depend, in part, on the health care financing and reimbursement policies of such countries. We cannot predict changes in health care systems in foreign countries, and therefore, do not know the effects on our business of possible changes. Shares eligible for future sale may adversely affect our ability to sell equity securities. Sales of our common stock (including the issuance of shares upon conversion of preferred stock) in the public market could materially and adversely affect the market price of shares because prior sales have been executed at or below our current market price. We have outstanding four series of preferred stock that convert to common stock at prices equivalent to $4.42, $4.00, $4.42 and $9.00, respectively, for our series A, series B, series C and series D convertible preferred stock. Our obligation to convert the preferred stock upon demand by the holders may depress the price of our common stock and also make it more difficult for us to sell equity securities or equity-related securities in the future at a time and price that we deem appropriate. As of June 4, 2004, we had 9,905,324 shares of common stock outstanding, plus (1) 80,400 shares of series A convertible preferred stock, convertible into approximately 454,750 shares of common stock at the conversion rate of 1:5.656, (2) 19,925 shares of series B Convertible Preferred stock convertible into approximately 124,531 shares of common stock at the conversion rate of 1:6.25, (3) 67,252 shares of series C convertible preferred stock convertible into approximately 380,384 shares of common stock at the conversion rate of 1:5.656, (4) 200,000 shares of series D convertible preferred stock convertible into approximately 555,540 shares of common stock at the conversion rate of 1:2.778, (5) 964,057 options to purchase shares of common stock with a weighted-average exercise price of $8.91 per share and (6) 2,885,312 warrants to purchase shares of common stock with a weighted-average exercise price of $7.42 Of the shares outstanding, 7,297,511 shares of common stock are freely tradable without restriction. All of the remaining 2,607,813 shares are restricted from resale, except pursuant to certain exceptions under the Securities Act of 1933, as amended (the "Securities Act"). -38- Our outstanding options and warrants may adversely affect our ability to consummate future equity financings due to the dilution potential to future investors. We have outstanding options and warrants for the purchase of shares of our common stock with exercise prices currently below market which may adversely affect our ability to consummate future equity financings. The holders of such warrants and options may exercise them at a time when we would otherwise be able to obtain additional equity capital on more favorable terms. To the extent any such options and warrants are exercised, the value of our outstanding shares of our common stock will be diluted. As of June 4, 2004, we have outstanding vested options to purchase 654,508 shares of common stock at a weighted-average exercise price of $7.24 and vested warrants to purchase 2,875,312 shares of common stock with a weighted-average price of $7.44. Due to the number of shares of common stock we are obligated to sell pursuant to outstanding options and warrants described above, potential investors may not purchase our future equity offerings at market price because of the potential dilution such investors may suffer as a result of the exercise of the outstanding options and warrants. The market price of our common stock has experienced significant volatility. The securities markets from time to time experience significant price and volume fluctuations unrelated to the operating performance of particular companies. In addition, the market prices of the common stock of many publicly traded pharmaceutical and biotechnology companies have been and can be expected to be especially volatile. Our common stock price in the 52-week period ended June 10, 2004 had a low of $5.35 and high of $32.51. Announcements of technological innovations or new products by us or our competitors, developments or disputes concerning patents or proprietary rights, publicity regarding actual or potential clinical trial results relating to products under development by us or our competitors, regulatory developments in both the United States and foreign countries, delays in our testing and development schedules, public concern as to the safety of pharmaceutical drugs or biologics and economic and other external factors, as well as period-to-period fluctuations in our financial results, may have a significant impact on the market price of our common stock. The realization of any of the risks described in these "Risk Factors" may have a significant adverse impact on such market prices. We routinely pay vendors in stock as consideration for their services; this may result in shareholder dilution, additional costs and difficulty retaining certain vendors. In order for us to preserve our cash resources, we often pay vendors in shares, warrants or options to purchase shares of our common stock rather than cash. Payments for services in stock may materially and adversely affect our shareholders by diluting the value of outstanding shares of our common stock. In addition, in situations where we have agreed to register the shares issued to a vendor, this will generally cause us to incur additional expenses associated with such registration. Paying vendors in shares, warrants or options to purchase shares of common stock may also limit our ability to contract with the vendor of our choice should that vendor decline payment in stock. -39- We do not intend to pay dividends on our common stock. Until such time as we pay cash dividends our stockholders must rely on increases in our stock price for appreciation. We have never declared or paid dividends on our common stock. We intend to retain future earnings to develop and commercialize our products and therefor we do not intend to pay cash dividends in the foreseeable future. Until such time as we determine to pay cash dividends on our common stock, our stockholders must rely on increases in our common stock's market price for appreciation. There are limitations on the liability of our directors, and we may have to indemnify our officers and directors in certain instances. Our certificate of incorporation limits, to the maximum extent permitted under Delaware law, the personal liability of our directors for monetary damages for breach of their fiduciary duties as directors. Our bylaws provide that we will indemnify our officers and directors and may indemnify our employees and other agents to the fullest extent permitted by law. We have entered into indemnification agreements with our officers and directors containing provisions that are in some respects broader than the specific indemnification provisions under Delaware law. The indemnification agreements may require us, among other things, to indemnify such officers and directors against certain liabilities that may arise by reason of their status or service as directors or officers (other than liabilities arising from willful misconduct of a culpable nature), to advance their expenses incurred as a result of any proceeding against them as to which they could be indemnified and to obtain directors' and officers' insurance. Section 145 of the Delaware General Corporation Law provides that a corporation may indemnify a director, officer, employee or agent made or threatened to be made a party to an action by reason of the fact that he or she was a director, officer, employee or agent of the corporation or was serving at the request of the corporation, against expenses actually and reasonably incurred in connection with such action if he or she acted in good faith and in a manner he or she reasonably believed to be in, or not opposed to, the best interests of the corporation, and, with respect to any criminal action or proceeding, had no reasonable cause to believe his or her conduct was unlawful. Delaware law does not permit a corporation to eliminate a director's duty of care and the provisions of our certificate of incorporation have no effect on the availability of equitable remedies, such as injunction or rescission, for a director's breach of the duty of care. We believe that our limitation of director liability assists us to attract and retain qualified directors. However, in the event a director or the board commits an act that may legally be indemnified under Delaware law, we will be responsible to pay for such director(s) legal defense and potentially any damages resulting therefrom. Furthermore, the limitation on director liability may reduce the likelihood of derivative litigation against directors, and may discourage or deter stockholders from instituting litigation against directors for breach of their fiduciary duties, even though such an action, if successful, might benefit us and our stockholders. Given the difficult environment and potential for incurring liabilities currently facing directors of publicly-held corporations, we believe that director indemnification is in our and our stockholders best interests because it enhances our ability to retain highly qualified directors and reduce a possible deterrent to entrepreneurial decision-making. -40- Nevertheless, limitations of director liability may be viewed as limiting the rights of stockholders, and the broad scope of the indemnification provisions contained in our certificate of incorporation and bylaws could result in increased expenses. Our board of directors believes, however, that these provisions will provide a better balancing of the legal obligations of, and protections for, directors and will contribute positively to the quality and stability of our corporate governance. Our board of directors has concluded that the benefit to stockholders of improved corporate governance outweighs any possible adverse effects on stockholders of reducing the exposure of directors to liability and broadened indemnification rights. Product liability exposure may expose us to significant liability. We do not have pharmaceutical products for sale and we therefor do not carry product liability insurance. However, if we do commercialize drug products we will face risk of exposure to product liability and other claims and lawsuits in the event that the development or use of our technology or prospective products is alleged to have resulted in adverse effects. We may not be able to avoid significant liability exposure. We may not have sufficient insurance coverage and we may not be able to obtain sufficient coverage at a reasonable cost. An inability to obtain product liability insurance at acceptable cost or to otherwise protect against potential product liability claims could prevent or inhibit the commercialization of our products. A product liability claim could hurt our financial performance. Even if we avoid liability exposure, significant costs could be incurred, potentially damaging our financial performance. We do carry commercial general liability insurance and clinical trials insurance which covers our human clinical trial activities. ITEM 2. PROPERTIES Our administrative offices and research laboratories are located at 150 Fairway Drive, Suite 150, Vernon Hills, Illinois 60061. We occupy approximately 9,750 square feet of space under a lease that expires on March 14, 2005. We are in the process of negotiating an extension on the current lease. Our rent for the Vernon Hills facility is $12,800 per month through March 2005. We are also charged by the landlord a portion of the real estate taxes and common area operating expenses. Our New York offices are located at One North End Avenue, New York, New York 10282. We pay rent of approximately $10,100 per month, on a month-to-month basis, for approximately 2,500 square feet of space for our New York office. (See Item 13. "Certain Relationships and Related Transactions.") We believe our current facilities are adequate for our needs for the foreseeable future and, in the opinion of our management, the facilities are adequately insured. Our indirectly wholly-owned subsidiary, Immtech Life Science, owns two floors of a newly-constructed building located in the Futian Free Trade Zone, Shenzhen, in the PRC in which we intend to construct a pharmaceutical production facility for manufacture of our products. The property comprises the first two floors of an industrial building named the Immtech Life Science Building. The duration of the land use right associated with the building on which the property is located is 50 years which expires May 24, 2051. -41- ITEM 3. LEGAL PROCEEDINGS We are parties to the following legal proceedings: Dale M. Geiss v. Immtech International, Inc. and Criticare Systems, Inc. ------------------------------------------------------------------------ On January 14, 2002 plaintiff filed a complaint in the Circuit Court of the Nineteenth Judicial Circuit, Lake County, State of Illinois, against the Company and Criticare Systems, Inc. ("Criticare"). The Company filed two motions to dismiss, both of which were successful. Thereafter, the plaintiff amended his complaint for a third time. After engaging in preliminary discovery, plaintiff agreed to voluntarily dismiss his action. On February 10, 2004, the Court entered an Order granting plaintiff's motion to voluntarily dismiss the action without prejudice. Immtech International, Inc., et al. v. Neurochem, Inc., et al. -------------------------------------------------------------- On August 12, 2003, the Company filed a lawsuit in Federal District Court in New York against Neurochem, Inc. On January 23, 2004, the Company amended the complaint and added two additional plaintiffs, UNC and Georgia State, and an additional defendant, Neurochem (International) Limited. The Company's amended complaint alleges that Neurochem misappropriated the Company's intellectual property by filing a series of patent applications relating to compounds synthesized and developed by the Consortium, with whom Immtech has an exclusive license agreement. The misappropriated intellectual property was provided to Neurochem pursuant to a testing agreement under which Neurochem agreed to test the compounds to determine if they could be successfully used to treat Alzheimer's disease. Pursuant to the terms of the agreement, Neurochem agreed to keep all information confidential, not to disclose or exploit the information without Immtech's prior written consent, to advise Immtech before filing any patent applications and to provide the Company with all testing and evaluation data. The amended complaint alleges that Neurochem fraudulently induced the Company into signing the testing agreement, misappropriated valuable intellectual property, filed a series of fraudulent patent applications, breached numerous provisions of the testing agreement, fraudulently transferred all its rights in the patent applications to an offshore affiliate - Neurochem (International) Limited, blocking the development of the Consortium's compounds for the treatment of Alzheimer's disease. By engaging in these acts, plaintiffs allege that defendants have prevented the public from obtaining the potential benefit of new drugs for the treatment of Alzheimer's disease, which would be in competition to Neurochem's Alzhemed drug. The plaintiffs seek injunctive relief and monetary and punitive damages. The defendants recently filed a motion with the court to compel arbitration, or in the alternative, to dismiss the amended complaint. After receiving legal memorandum from the parties and having heard oral argument, on April 8, 2004, the court ruled that an arbitrator, not the court, should decide the issue of whether the Company's claims against the defendants should be heard by the court or an arbitrator. The Company has requested the court reconsider its ruling, or in the alternative, issue an order allowing the Company to file an appeal to the Second Circuit Court of Appeals. Defendants have opposed the Company's motion, and the issue is currently before the court. -42- Gerhard Von der Ruhr et al. v. Immtech International, Inc. et. al. ------------------------------------------------------------------ On October 20, 2003, plaintiffs filed a complaint in the United States District Court for the Northern District of Illinois against the Company and certain officers and directors. On April 19, 2004, the Company and its officers and directors filed a motion with the court to dismiss the complaint. On May 17, 2004, plaintiffs filed opposition papers. Defendants have filed a reply brief and the motion is currently before the court. The Company believes that plaintiffs' claims are meritless and intends to vigorously defend this action. ITEM 4. SUBMISSION OF MATTERS TO A VOTE OF SECURITY HOLDERS Matters submitted to a vote of the security holders at our Annual Meeting on January 7, 2004 at the American Stock Exchange in New York City have been disclosed in our quarterly report on Form 10-Q for the quarter ended December 31, 2003, filed with the SEC on February 17, 2004. PART II. ITEM 5. MARKET FOR REGISTRANT'S COMMON EQUITY AND RELATED STOCKHOLDER MATTERS Market Information ------------------ Our common stock has been quoted on the American Stock Exchange under the symbol "IMM" since August, 11, 2003 (our common stock was quoted under the Symbol "IMMT" on the NASDAQ SmallCap Market from April 26, 1999 to March 29, 2000, on the NASDAQ National Market System from March 30, 2000 to March 8, 2002, on the NASDAQ SmallCap Market from March 9, 2002 to December 2, 2002, and on the NASDAQ OTC Bulletin Board from December 2, 2002 to August 11, 2003). Following are the reported high and low share trade prices as reported by IDD Information Services, NASDAQ Online and Lexis/Nexis for each of the quarters set forth below since the fiscal quarter ended March 31, 2002. High Low ------- ------- 2002 Quarter ended March 31, 2002 $ 7.400 $ 4.000 Quarter ended June 30, 2002 $ 5.990 $ 2.800 Quarter ended September 30, 2002 $ 5.150 $ 2.390 Quarter ended December 31, 2002 $ 3.800 $ 2.120 2003 Quarter ended March 31, 2003 $ 4.850 $ 1.580 Quarter ended June 30, 2003 $ 7.000 $ 4.150 Quarter ended September 30, 2003 $18.820 $ 5.700 Quarter ended December 31, 2004 $32.510 $ 9.000 2004 Quarter ended March 31, 2004 $19.500 $10.110 -43- Shareholders ------------ As of June 4, 2004, there were approximately 232 shareholders of record of our common stock and the number of beneficial owners of shares of common stock as of such date was approximately 2,854. As of June 4, 2004, there were approximately 9,905,324 shares of common stock issued and outstanding. Dividends --------- We have never declared or paid dividends on our common stock and we do not intend to pay any common stock dividends in the foreseeable future. Our Series A Convertible Preferred Stock, Series B Convertible Preferred Stock, Series C Convertible Preferred Stock and Series D Convertible Preferred Stock earn dividends of 6%, 8%, 8% and 6% per annum, respectively, each payable semi-annually on each April 15 and October 15 while outstanding, and which, at our option, may be paid in cash or in shares of our common stock. On April 15, 2003, October 15, 2003 and April 15, 2004 we paid dividends to the holders of our Series A Convertible Preferred Stock and Series B Convertible Preferred Stock on October 15, 2003 and April 15, 2004 with paid dividends to the holders of our Series C Convertible Preferred Stock, and on April 15, 2004 we paid dividends to the holders of our Series D Convertible Preferred Stock, in each case in shares of common stock, with fractional shares paid in cash. Recent Sales of Unregistered Securities --------------------------------------- We issued unregistered securities in the following transactions during the fiscal quarter ended March 31, 2004: o On January 22, 2004 we issued (i) 24,600 shares of our Series D Stock and related warrants to purchase 24,600 shares of our common stock pursuant to an exemption from registration under Regulation D of the Securities Act for $615,000 in the aggregate and (ii) 175,400 shares of our Series D Stock and related warrants to purchase 175,400 shares of our common stock pursuant to an exemption from registration under Regulation S of the Securities Act for $4,385,000 in the aggregate. A complete description of the designations, preferences, voting powers, qualifications, special or relative rights and privileges of the Series D Stock is contained in our Series D Convertible Preferred Stock Certificate of Designation and a complete description of the terms of the warrants are contained in our form of Common Stock Warrant, both filed as exhibits to our current report on Form 8-K dated January 22, 2004. o On February 24, 2004 we issued 13,550 shares of common stock from the exercise of options by Craig B. Thompson, having received $6,328 for their exercise. -44- o On March 30, 2004 we issued 300 shares of common stock from the exercise of options by Regina Durlak, having received $765 for their exercise. -45- Securities Authorized for Issuance under Equity Compensation Plans ------------------------------------------------------------------ The following table provides information as of March 31, 2004, regarding compensation plans (including individual compensation arrangements) under which our equity securities are authorized for issuance. Number of securities remaining available for future issuance Number of under equity securities to Weighted average compensation be issued upon exercise price of plans exercise of outstanding (excluding outstanding options, securities options, warrants and reflected in Plan category (in warrants and rights rights(1) column(a)) thousands) (a) (b) (c) ----------------------- ------------------- ------------------ --------------- Equity compensation 962,574 $ 8.63 340,250 plans approved by security holders(2) Equity compensation 2,987,710 $ 7.70 plans not approved by security holders(3) ------------------------------------------------------- Total 3,950,284 $ 7.93 340,250 -------------------------------------------------------------------------------- ------------ (1) As adjusted for reverse stock splits that occurred on each of July 24, 1998 and January 25, 1999. (2) This category consists solely of options. (3) This category consists solely of warrants. Series C Convertible Preferred Stock Private Placements ------------------------------------------------------- On June 6, 2003, we filed a Series C Convertible Preferred Stock Certificate of Designation ("Series C Certificate of Designation") with the Secretary of State of the State of Delaware, designating 160,000 shares of our 5,000,000 authorized shares of preferred stock as Series C Convertible Preferred Stock, $0.01 par value, with a stated value of $25.00 per share ("Series C Preferred Stock"). Dividends on the Series C Preferred Stock accrue at a rate of 8% on the $25.00 stated value per share and are payable semi-annually on April 15 and October 15 of each year while the shares are outstanding. We have the option to pay the dividend either in cash or in equivalent shares of common stock. If common stock is to be used to pay the dividend, such common stock is to be valued at the 10-day volume-weighted average price immediately prior to the date of payment. Each share of Series C Preferred Stock is convertible by the holder at any time into shares of our common stock at a conversion rate determined by dividing the $25.00 stated value, plus any accrued and unpaid dividends (the "Liquidation Price"), by a $4.42 conversion price (the "Conversion Price"), subject to antidilution adjustment. We may at any time after the first anniversary of the date of issuance require that any or all outstanding shares of Series C Preferred Stock be converted into shares of our common stock, provided that the shares of -46- common stock into which the Series C Preferred Stock is convertible is registered pursuant to an effective registration statement. The number of shares of common stock will be determined by (i) dividing the Liquidation Price by the Conversion Price, provided that the closing bid price for our common stock exceeds $9.00 for 20 consecutive trading days within 180 days prior to notice of conversion, or (ii) if the requirements of (i) above are not met, the number of shares of common stock is determined by dividing 110% of the Liquidation Price by the Conversion Price. The Conversion Price is subject to antidilution adjustments, as set forth in the Series C Certificate of Designation. We may, upon 30 days' notice, redeem any or all outstanding shares of the Series C Preferred Stock by payment of the Liquidation Price to the holder of such shares, provided that the holder does not convert the Series C Preferred Stock into shares of common stock during the 30-day period. The Series C Preferred Stock has a preference in liquidation equal to $25.00 per share, plus any accrued and unpaid dividends. Each issued and outstanding share of Series C Preferred Stock is entitled to 5.6561 votes with respect to any and all matters presented to our stockholders for their action or consideration. Except as provided by law or by the provisions establishing any other series of preferred stock, holders of our Series A Convertible Preferred Stock, Series B Convertible Preferred Stock, Series C Preferred Stock and Series D Preferred Stock vote together with the holders of our common stock as a single class. From June 6, 2003 through June 9, 2003, we issued an aggregate of 125,352 shares of our Series C Preferred Stock in private placements to certain accredited and non-U.S. investors in reliance on Regulation D and Regulation S, respectively, under the Securities Act of 1933, as amended (the "Securities Act"). The gross proceeds of the offering were $3,133,800 as of June 18, 2003. The securities were sold pursuant to exemptions from registration under the Securities Act and we intend to register the shares under the Securities Act. Subject to adjustment for dilution, each share of Series C Preferred Stock is convertible into 5.6561 shares of common stock. Series D Convertible Preferred Stock Private Placements ------------------------------------------------------- On January 15, 2004, we filed a Series D Convertible Preferred Stock Certificate of Designation ("Series D Certificate of Designation") with the Secretary of State of the State of Delaware, designating 200,000 shares of our 5,000,000 authorized shares of preferred stock as Series D Convertible Preferred Stock, $0.01 par value, with a stated value of $25.00 per share ("Series D Preferred Stock"). Dividends on the Series D Preferred Stock accrue at a rate of 6% on the $25.00 stated value per share and are payable semi-annually on April 15 and October 15 of each year while the shares are outstanding. We have the option to pay the dividend either in cash or in equivalent shares of common stock. If common stock is to be used to pay the dividend, such common stock is to be valued at the 10-day volume-weighted average price immediately prior to the date of payment. Each share of Series D Preferred Stock is convertible by the holder at any time into shares of our common stock at a conversion rate determined by dividing the $25.00 stated value, plus any accrued and unpaid dividends (the "Liquidation Price"), by a $9.00 conversion price (the "Conversion Price"), subject to antidilution adjustment. We may at any time after -47- January 1, 2005 require that any or all outstanding shares of Series D Preferred Stock be converted into shares of our common stock, provided that the shares of common stock into which the Series D Preferred Stock is convertible is registered pursuant to an effective registration statement. The number of shares of common stock will be determined by (i) dividing the Liquidation Price by the Conversion Price, provided that the closing bid price for our common stock exceeds $18.00 for 20 consecutive trading days within 180 days prior to notice of conversion, or (ii) if the requirements of (i) above are not met, the number of shares of common stock is determined by dividing 110% of the Liquidation Price by the Conversion Price. The Conversion Price is subject to antidilution adjustments, as set forth in the Series D Certificate of Designation. We may, upon 30 days' notice, redeem any or all outstanding shares of the Series D Preferred Stock by payment of the Liquidation Price to the holder of such shares, provided that the holder does not convert the Series C Preferred Stock into shares of common stock during the 30-day period. The Series D Preferred Stock has a preference in liquidation equal to $25.00 per share, plus any accrued and unpaid dividends. Each issued and outstanding share of Series D Preferred Stock is entitled to 2.7778 votes with respect to any and all matters presented to our stockholders for their action or consideration. Except as provided by law or by the provisions establishing any other series of preferred stock, holders of our Series A Convertible Preferred Stock, Series B Convertible Preferred Stock, Series C Convertible Preferred Stock and Series D Convertible Preferred Stock vote together with the holders of our common stock as a single class. On January 15, 2004, we issued an aggregate of 200,000 shares of our Series D Preferred Stock in a private placement to certain accredited and non-U.S. investors in reliance on Regulation D and Regulation S, respectively, under the Securities Act of 1933, as amended (the "Securities Act"). The gross proceeds of the offering were $5,000,000. The securities were sold pursuant to exemptions from registration under the Securities Act and we intend to register the shares under the Securities Act. Subject to adjustment for dilution, each share of Series D Preferred Stock is convertible into 2.7778 shares of common stock. In January 2004, in connection with the Series D Convertible Preferred Stock private placement offering, we issued warrants to purchase 200,000 shares of our common stock at an exercise price of $16.00 per share of common stock. The warrants expire on the fifth anniversary of their date of issuance. The warrant exercise period commenced immediately upon issuance of the warrant. At any time after the first anniversary of the date of issuance and if our common stock closing price is above 200% of the exercise price for 20 consecutive trading days, we may, upon 20 days notice, redeem any unexercised portion of any warrants for a redemption fee equal to $.10 per share of common stock underlying the warrants. During the 20-day notice period, the warrant holder may exercise all or a portion of the warrants by tendering the appropriate exercise price. -48- Conversion of Preferred Stock to Common Stock. ---------------------------------------------- Series A. On May 10, 2004, holders of Series A Convertible Preferred Stock ("Series A Stock") converted 400 shares of Series A Stock and accrued dividends into 2,264 shares of common stock, respectively. Series C. On February 3, 2004, February 6, 2004, February 23, 2004, February 24, 2004, April 15, 2004, April 16, 2004, and May 10, 2004, holders of Series C Convertible Preferred Stock ("Series C Stock") converted 5,200 shares, 2,800 shares, 1,768 shares, 1,000 shares, 3,768 shares, 884 shares and 400 shares of Series C stock and accrued dividends into 29,627 shares, 15,953 shares, 10,095 shares, 5,711 shares, 21,311 shares, 5,000 shares, and 2,264 shares of common stock, respectively. Amendment to Restated Certificate of Incorporation -------------------------------------------------- On November 4, 2003, our Board of Directors authorized an amendment to our Restated Certificate of Incorporation to increase the number of authorized shares of common stock from 30 million to 100 million. This amendment was approved by our shareholders at the Company's annual meeting held on January 7, 2004. Additionally, the shareholders approved additional amendments to our Restated Certificate of Incorporation which provide for indemnification of our officers and directors to the maximum extent of Delaware law and to generally update our Restated Certificate of Incorporation as permitted by Delaware law. Our shareholders also authorized up to a two-for-one stock split of our common stock that our Board of Directors has so far deferred to act upon. The Board of Directors has determined that a stock split in not in our best interest at this time but reserves the right to implement the stock split as approved at such time as it deems prudent, if at all. ITEM 6. SELECTED FINANCIAL DATA The following table sets forth certain selected financial data that was derived from our financial statements (dollars in thousands except per share data): -49- Year ended March 31, ---------------------------------------------------------------------------------- ---------------------------------------------------------------------------------- 2004 2003 2002 2001 2000 ----------- ----------- ----------- ----------- ----------- Statement of Operations: REVENUES $ 2,416 $ 1,609 $ 3,522 $ 1,355 $ 369 EXPENSES: Research and development 3,293 2,570 (3)3,958 6,695 (1)10,255 General and administrative (6)11,989 (5)3,732 2,928 (2)4,719 1,732 Equity in loss of joint venture 135 ----------- ----------- ----------- ----------- ----------- Total expenses 15,282 6,302 6,886 11,414 12,122 LOSS FROM OPERATIONS (12,866) (4,693) (3,364) (10,059) (11,753) ----------- ----------- ----------- ----------- ----------- OTHER INCOME(EXPENSE): Interest income 20 14 41 199 319 Loss on sales of investment securities - net ----------- ----------- ----------- ----------- ----------- Other income (expense) - net 20 14 41 196 319 ----------- ----------- ----------- ----------- ----------- NET LOSS (12,866) (4,679) (3,323) (9,863) (11,434) CONVERTIBLE PREFERRED STOCK DIVIDENDS AND CONVERTIBLE PREFERRED STOCK DEEMED DIVIDENDS(4) (3,526) (452) (938)(4) REDEEMABLE PREFERRED STOCK CONVERSION, PREMIUM AMORTIZATION AND DIVIDENDS ----------- ----------- ----------- ----------- ----------- NET LOSS ATTRIBUTABLE TO COMMON STOCKHOLDERS (16,372) $ (5,131) $ (4,261) $ (9,863) $ (11,434) =========== =========== =========== =========== =========== -50- Year ended March 31, ---------------------------------------------------------------------------------- ---------------------------------------------------------------------------------- 2004 2003 2002 2001 2000 ----------- ----------- ----------- ----------- ----------- BASIC AND DILUTED NET LOSS PER SHARE ATTRIBUTABLE TO COMMON STOCKHOLDERS: ----------- ----------- ----------- ----------- ----------- Net loss (1.43) (0.71) (0.55) (1.78) (2.27) Convertible preferred stock dividends and convertible preferred stock premium deemed dividends (0.39) (0.07) (0.16) ----------- ----------- ----------- ----------- ----------- BASIC AND DILUTED NET LOSS PER SHARE ATTRIBUTABLE TO COMMON STOCKHOLDERS $ (1.82) $ (0.78) $ (0.71) $ (1.78) $ (2.27) =========== =========== =========== =========== =========== WEIGHTED AVERAGE SHARES USED IN COMPUTING BASIC AND DILUTED LOSS PER SHARE 8,977,817 6,565,495 6,011,416 5,545,190 5,036,405 -51- March 31, ---------------------------------------------------------------------------------- ---------------------------------------------------------------------------------- 2004 2003 2002 2001 2000 ----------- ----------- ----------- ----------- ----------- Balance Sheet Data: Cash and cash equivalents 6,745 112 2,038 2,098 4,596 Restricted funds on deposit 2,155 2,740 602 3,813 Investment securities available for sale 1,361 Working capital (deficiency) 6,136 (115) 1,567 663 4,402 Total assets 12,586 6,610 2,876 6,168 6,224 Convertible preferred stock 9,522 5,138 4,032 Deficit accumulated during development stage (58,539) (42,167) (37,036) (32,775) (22,912) =========== =========== =========== =========== =========== Stockholders' equity 9,748 3,192 1,736 859 4,620 ----------- (1) Includes $6,113 of research and development costs related to the acquisition of rights to technology and dications which were acquired through the issuance of 611,250 shares of common stock. (2) Includes $1,288 of costs related to the issuance of warrants to purchase 300,000 shares of common stock as compensation for financial consulting services. (3) Includes $1,159 credit to (reduction in) research and development costs for the settlement of certain disputed costs previously expensed during the year ended March 31, 2000. (4) See Note 7 to Notes to Financial Statements for a discussion on the convertible preferred stock dividends. (5) Includes $758 of costs related to the issuance of 150,000 shares of common stock to Cheung Ming Tak to act as our non-exclusive agent to develop and qualify potential strategic partners for the purpose of testing and/or the commercialization of Company products in the PRC; $188 of costs related to the issuance of 40,000 shares of common stock to The Gabriele Group, L.L.C., for assistance with respect to management consulting, strategic planning, public relations and promotions and includes $89 of costs related to the issuance of 8,333 shares of common stock and the vesting of 29,165 warrants to Fulcrum Holdings of Australia, Inc. ("Fulcrum"). (6) Includes non-cash charges of (i) $2,744 of costs related to the issuance of warrants to purchase 600,000 shares of common stock issued to China Harvest International Ltd as payment for services to assist in obtaining regulatory approval to conduct clinical trials in China, (ii) $63 for the issuance of 10,000 shares of common stock issued to Mr. David Tat Koon Shu for consulting services in China, (iii) $1,400 for the issuance of 100,000 shares of common stock issued to Fulcrum for assisting with listing our securities on a recognized stock exchange and for consulting services, (iv) $2,780 for the vested portion of 91,667 shares of common stock and the vested portion of warrants to purchase 320,835 shares of common stock issued to Fulcrum during the fiscal year based on agreements signed March 21, 2003, and (v) $247 for the attainment of certain milestones with respect to the vesting of warrants to purchase 20,000 shares of common stock issued to Pilot Capital Group, LLC (f/k/a The Gabriele Group, LLC) based upon agreements signed July 31, 2002. -52- ITEM 7. MANAGEMENT'S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS OF OPERATIONS Overview We are a pharmaceutical company focused on the development and commercialization of oral drugs to treat infectious diseases and metabolic disorders. We have development programs that include fungal infections, malaria, tuberculosis, diabetes, Pneumocystis carinii pneumonia and tropical medicine diseases, including African sleeping sickness (trypanosomiasis) and leishmaniasis. We hold worldwide patents, patent applications, and licenses to worldwide patents, patent applications and technologies from a scientific consortium and exclusive rights to commercialize products from patents and licenses that are integral to our business. We intend to work with our scientific and foundation partners to validate our technology platform, illustrating dications' low toxicity, broad application, and oral deliverability. We plan in the near future to sell drugs for compassionate use in niche markets as we further develop drugs to target multi-billion dollar markets such as antifungal, TB, diabetes and cancer treatments. As a validation of our efforts, the United States Food and Drug Administration ("FDA") has granted "fast-track" designation of DB289 for treatment of African sleeping sickness. Fast-track designation allows for expedited FDA regulatory review of DB289 for African sleeping sickness. Since our formation in October 1984, we have engaged in research and development programs, expanding our network of scientists and scientific advisors, licensing technology agreements and advancing the commercialization of the dication technology platform. To minimize shareholders' dilution, we use foundation and government grants, the expertise and resources of strategic partners and third parties in a number of areas, including (i) laboratory research, (ii) pre-clinical and human clinical trials and (iii) manufacture of pharmaceutical drugs. We have licensing and exclusive commercialization rights to a dicationic anti-infective pharmaceutical platform and are developing drugs intended for commercial use based on that platform. Dication pharmaceutical drugs (structural class defined by molecules with positive charges on each end held together by a linker) work by blocking life-sustaining enzymes from binding to the key sites in the "minor groove" of an organism's DNA, thereby killing the infectious organisms that cause fungal, parasitic, bacterial and viral diseases. The key site on an organism's DNA is an area where enzymes interact with the infectious organism's DNA as part of their normal life cycle. Structurally, dications are chemical molecules that have two positively charged ends held together by a chemical linker. The composition of the dications, with positive charges on both ends (shaped like molecular barbells) allows dications to bind (similar to a band-aid) to the negatively charged key sites of an infectious microorganism's DNA. The bound dications block the life-sustaining enzymes from attaching to the DNA's key sites, thereby killing the infectious organism. With the exception of certain research funding agreements and certain grants, we have not generated any revenue from operations. For the period from inception (October 15, 1984) to March 31, 2004, we incurred cumulative net losses of approximately $55,993,000. We have incurred additional losses since such date and we expect to incur additional operating losses -53- for the foreseeable future. We expect that our cash sources for at least the next year will be limited to: o payments from The University of North Carolina at Chapel Hill, charitable foundations and other research collaborators under arrangements that may be entered into in the future; and o research grants, such as Small Business Technology Transfer Program ("STTR") grants and Small Business Innovation Research ("SBIR") grants; o borrowing funds or the issuance of securities. The timing and amounts of grant and payment revenues, if any, will likely fluctuate sharply and depend upon the achievement of specified milestones, and results of operations for any period may be unrelated to the results of operations for any other period. Critical Accounting Policies and Estimates Our significant accounting policies are described in Note 1 to the Notes to the Consolidated Financial Statements. These financial statements have been prepared in accordance with accounting principles generally accepted in the United States. The preparation of these financial statements requires us to make estimates and judgments that affect the reported amounts of assets, liabilities, revenues and expenses, and related disclosure of contingent liabilities. On an ongoing basis, we evaluate our estimates, including those related to the fair value of our preferred and common stock and related options and warrants, the recognition of revenues and costs related to our research contracts, and the useful lives or impairment of our property and equipment. We base our estimates on historical experience and on various other assumptions that we believe to be reasonable under the circumstances, the results of which form the basis of judgments regarding the carrying values of assets and liabilities that are not readily apparent from other sources. Actual results may differ from these estimates under different assumptions or conditions. Grants to perform research are our primary source of revenue and are generally granted to support research and development activities for specific projects or drug candidates. Revenue related to grants to perform research and development is recognized as earned based on the performance requirements of the specific grant. Upfront cash payments from research and development grants are reported as deferred revenue until such time as the research and development activities covered by the grant are performed. We use the intrinsic-value method of accounting for stock based awards granted to employees in accordance with Accounting Principles Board Opinion No. 25 and its related interpretations. We record stock based compensation expense for non-employees at the fair value of the options or warrants granted in accordance with Statement of Financial Accounting Standards No. 123 ("SFAS 123") and Emerging Issues Task Force No. 96-18 ("EITF 96-18"). The fair value of options granted to non-employees is estimated using a Black-Scholes option valuation model. The model considers a number of factors, including the market price and volatility of our common stock at the date of measurement. We measure the compensation expense for options and warrants granted to non-employees as the underlying options vest. The compensation expense related to all grants is being amortized using the graded vesting method, in accordance with SFAS 123, EITF 96-18 and FASB Interpretation No. 28, over the vesting period of each respective stock option. We believe that the accounting policies affecting these estimates are our critical accounting policies. Research and Development Expenses All research and development costs are expensed as incurred. Research and development expenses include, but are not limited to, payroll and personnel expenses, lab supplies, preclinical studies, raw materials to manufacture clinical trial drugs, manufacturing costs, sponsored research at other labs, consulting, and research-related overhead. Accrued liabilities for raw materials to manufacture clinical trial drugs, manufacturing costs, and sponsored research reimbursement fees are included in accrued liabilities and included in research and development expenses. Specific information pertaining to each of our major -54- research and development projects follows. This information includes to the extent ascertainable project status, costs incurred for the relevant fiscal years (including costs to date), nature, timing and estimated costs of project completion, anticipated completion dates, and the period in which material net cash inflows from projects is expected to commence, if at all. All of our research and development projects contain high levels of risk. Even if development is completed on schedule, there is no guarantee that any of our products will be licensed for sale. Human trials conducted in foreign and developing countries have additional risks, including governmental and local militia uprisings that may interrupt or displace our work. We are unable to quantify the impact to our operations, financial position or liquidity if we are unable to complete on schedule, or at all, any of our product commercialization programs. Malaria We expensed research and development costs for our Malaria program for the fiscal years ended March 31, 2002, March 31, 2003 and March 31, 2004 of approximately $0, $45,000, and $250,000 respectively. Since our inception through May 2004, approximately $318,000 has been expensed on research and development for the malaria project. Pneumocystis carinii pneumonia ("PCP") We expensed research and development costs for the PCP program for the fiscal years ended March 31, 2002, March 31, 2003, and March 31, 2004 of approximately $30,000, $194,000 and $241,000, respectively. Since our inception through May 2004, approximately $471,000 has been expensed on the PCP program. Trypanosomiasis Research and development costs expensed by the Company for our trypanosomiasis program for the fiscal years ended March 31, 2002, March 31, 2003, and March 31, 2004 have been approximately $2,530,000, $1,228,000 and $2,018,000, respectively. Since our inception through May 2004, approximately $6,637,000 has been expensed on the trypanosomiasis program. Antifungal Program & Tuberculosis ("TB") Each of the antifungal and TB studies is estimated to cost between $25-40 million dollars (including manufacturing and formulation of their respective drugs). The Company is unable to calculate when initial drug sales for the antifungal and TB treatments may commence because of the early stage of development. We expensed research and development costs for the antifungal program for the fiscal years ended March 31, 2002, March 31, 2003, and March 31, 2004 of approximately $0, $1,000 and $32,000, respectively. Since our inception through May 2004, approximately $367,000 has been expensed on the antifungal program. We expensed research and development costs for the TB program for the fiscal years ended March 31, 2002, March 31, 2003 and March 31, 2004 of approximately $50,000, -55- $10,000 and $24,000 respectively. Since our inception through May 2004, approximately $104,000 has been expensed. Pharmaceutical Cancer Program We expensed research and development costs for the pharmaceutical cancer program for the fiscal years ended March 31, 2002, March 31, 2003, and March 31, 2004 of approximately $0, $0 and $0, respectively. Since our inception through May 2004, approximately $24,000 has been expensed on the pharmaceutical cancer program. Liquidity and Capital Resources From our inception through March 31, 2004, we have financed our operations with: o proceeds from various private placements of debt and equity securities, an initial public offering and other cash contributed from stockholders, which in the aggregate raised approximately $39,258,000; o payments from research agreements, foundation grants and SBIR grants and STTR program grants of approximately $11,259,000; and o the use of stock, options and warrants in lieu of cash compensation. On January 22, 2004, we sold in private placements pursuant to Regulation D and Regulation S of the Securities Act of 1933, as amended ("Securities Act") (i) 200,000 shares of our Series D Convertible Preferred Stock, $0.01 par value ("Series D Stock") at a stated value of $25.00 per share and (ii) warrants to purchase 200,000 shares of our common stock with a $16.00 per share exercise price, for the aggregate consideration of $5,000,000 before issuance cost. The net proceeds were approximately $4,571,000. Each share of Series D Stock, among -56- other things, (i) earns a 6% dividend payable, at our discretion, in cash or common stock, (ii) has a $25.00 (plus accrued but unpaid dividends) liquidation preference pari passu with our other outstanding preferred stock, (iii) is convertible into 2.7778 shares of common stock and (iv) may be converted to common stock by us any time after January 1, 2005. The related warrants expire five years from the date of grant. From June 6, 2003 through June 9, 2003, we issued an aggregate of 125,352 shares of our Series C Preferred Stock in private placements to certain accredited and non-U.S. investors in reliance on Regulation D and Regulation S, respectively, under the Securities Act. The securities were sold pursuant to exemptions from registration under the Securities Act and were subsequently registered on Form S-3 (Registration Statement No. 333-108278). The gross proceeds of the offering were $3,133,800 and the net proceeds were approximately $2,845,000. On September 25, 2002 and October 28, 2002, we issued an aggregate of 76,725 shares of our Series B Convertible Preferred Stock and 191,812 related warrants in private placements to certain accredited and non-U.S. investors in reliance on Regulation D and Regulation S, respectively, under the Securities Act. The warrants have an exercise period of five years from the date of issuance and an exercise price of 6.125 per share. The securities were sold pursuant to exemptions from registration under the Securities Act and were subsequently registered on Form S-3 (Registration Statement No. 333-101197). The gross proceeds of the offering were $1,918,125 and the net proceeds were approximately $1,859,000. On February 14, 2002 and February 22, 2002, we issued an aggregate of 160,100 shares of our Series A Convertible Preferred Stock and 400,250 related warrants in private placements to certain accredited and non-U.S. investors in reliance on Regulation D and Regulation S, respectively, under the Securities Act. In connection with this offering, we issued in the aggregate 60,000 shares of common stock and 760,000 warrants to purchase shares of common stock to consultants assisting in the private placements. The warrants have an exercise period of five years from the date of issuance and exercise prices of (i) $6.00 per share for 500,000 warrants, (ii) $9.00 per share for 130,000 warrants and (iii) $12.00 per share for 130,000 warrants. The $9.00 and $12.00 warrants will not vest, and therefore will not be exercisable, unless our common stock meets or exceeds the respective exercise price for 20 consecutive trading days prior to January 31, 2003. The gross proceeds of the offering were $4,003,000 and the net proceeds were $3,849,000. On December 8, 2000, we completed a private placement offering that raised net proceeds of approximately $4,306,000 of additional net equity capital through the issuance of 584,250 shares of common stock. On April 26, 1999, we issued 1,150,000 shares of common stock through an initial public stock offering ("IPO"), resulting in net proceeds of approximately $9,173,000. The underwriters received warrants to purchase 100,000 additional shares of common stock at $16.00 per share. Those warrants expired on April 25, 2004. We used $110,000 of the net proceeds of the IPO to repay amounts due to the State of Illinois and Northwestern University. Substantially all of the remaining net proceeds of the IPO were used to fund our research and development efforts, including clinical and pre-clinical studies. Any net proceeds not applied to our research -57- and development efforts were used for working capital and general corporate purposes, including hiring additional employees. Our cash resources have been used to finance research and development, including sponsored research, capital expenditures, expenses associated with the efforts of the Scientific Consortium and general and administrative expenses. Over the next several years, we expect to incur substantial additional research and development costs, including costs related to early-stage research in pre-clinical and clinical trials, increased administrative expenses to support research and development operations and increased capital expenditures for expanded research capacity, various equipment needs and facility improvements or relocation. As of March 31, 2004, we had federal net operating loss carryforwards of approximately $42,840,000, which expire from 2006 through 2024. We also had approximately $41,092,000 of stated net operating loss carryforwards as of March 31, 2004, which expire from 2009 through 2024, available to offset certain future taxable income for state (primarily Illinois) income tax purposes. Because of "change of ownership" provisions of the Tax Reform Act of 1986, approximately $920,000 of our net operating loss carryforwards for federal purposes are subject to an annual limitation regarding utilization against taxable income in future periods. As of March 31, 2004, we had federal income tax credit carryforwards of approximately $750,000, which expire from 2008 through 2024. We believe our existing resources, but not including proceeds from any grants we may receive, are sufficient to meet our planned expenditures through June 2005, although there can be no assurance that we will not require additional funds. In addition, we anticipate the receipt of approximately an additional $3.2 million payment (restricted funds) under the Clinical Research Subcontract with the University of North Carolina at Chapel Hill ("UNC") (funded by The Gates Foundation) and approximately an additional $2.7 million under the agreement with MMV in calendar year 2004. Our working capital requirements will depend upon numerous factors, including the progress of our research and development programs (which may vary as product candidates are added or abandoned), pre-clinical testing and clinical trials, achievement of regulatory milestones, our corporate partners fulfilling their obligations to us, the timing and cost of seeking regulatory approvals, the level of resources that we devote to the development of manufacturing, our ability to maintain existing, and establish new, collaborative arrangements with other companies to provide funding to us to support these activities and other factors. In any event, we will require substantial funds in addition to our existing working capital to develop our product candidates and otherwise to meet our business objectives. We have, through our purchase of Super Insight Limited, obtained an ownership interest in improved real property on which we intend to construct a pharmaceutical manufacturing facility. We plan to purchase and install a pharmaceutical production line for which we have received estimates of $8 to $12 million from several consultants for the initial equipment and installation based on requirements for capacity and quality supplied by us. We are seeking partners both in the PRC and domestically to fund part or all of the capital cost of construction of the pharmaceutical production line. Payments Due under Contractual Obligations We have future commitments at March 31, 2004 consisting of operating lease obligations as follows: Year Ending Lease Payments March 31, 2005 $153,000 -------- Total $153,000 -58- Results of Operations Year Ended March 31, 2004 Compared with Year Ended March 31, 2003 Revenues under collaborative research and development agreements were approximately $2,416,000 and $1,609,000 in the years ended March 31, 2004 and 2003, respectively. In 2004, we recognized revenues of approximately $2,114,000 relating to the clinical research subcontract agreement between us and UNC funded by a grant that UNC received from The Gates Foundation, and approximately $302,000 relating to the testing agreement with MMV, while in 2003, there were revenues recognized of approximately $1,389,000 relating to the clinical research subcontract agreement, grant revenues of approximately $70,000 from SBIR grants from the NIH and revenues of $150,000 relating to the Confidentiality, Testing and Option Agreement with Neurochem Inc., a Canadian company. Research and development expenses increased from approximately $2,570,000 in 2003 to approximately $3,293,000 in 2004. Expenses relating to the clinical research subcontract agreement with UNC increased from approximately $1,294,000 in 2003 to approximately $2,099,000 in 2004. The initiation of the MMV testing agreement in 2004 accounted for expenses of approximately $301,000. Expenses relating to pre-clinical and clinical trial costs primarily for Pneumocystis carinii pneumonia decreased from approximately $442,000 in 2003 to approximately $198,000 in 2004. The decrease in expenses for Pneumocystis carinii pneumonia was primarily due to the payment of start up costs to a contract research organization in South Africa and Peru in 2003 which were not incurred in 2004. Other research and development costs relating primarily to SBIR's and obligations to UNC decreased from approximately $329,000 in 2003 to approximately $190,000. General and administrative expenses were approximately $11,990,000 in 2004, compared to approximately $3,732,000 in 2003. The increase in general and administrative expenses was primarily due to non-cash expenses for common stock, stock options and warrant issuance in 2004 of approximately $7,234,000 as compared to approximately $1,035,000 in 2003. Non-cash expenses in 2004 included (i) approximately $2,744,000 for the issuance of a warrant to purchase 600,000 shares of common stock issued to China Harvest International Ltd. as payment for services to assist us in obtaining regulatory approval to conduct clinical trials in China, (ii) approximately $63,000 for the issuance of 10,000 shares of common stock issued to Mr. David Tat Koon Shu for consulting services in China, (iii) approximately $1,400,000 for the issuance of 100,000 shares of common stock issued to Fulcrum for assistance with listing our securities on a recognized stock exchange and for consulting services, (iv) approximately $2,780,000 for the vested portion of 91,667 shares of common stock and the vested portion of warrants to purchase 320,835 shares of common stock issued to Fulcrum during the fiscal year based on agreements signed March 21, 2003 and (v) approximately $247,000 for the reaching of certain milestones which resulted in the vesting of a warrant to purchase 20,000 shares of common stock issued to Pilot Capital Group, LLC (f/k/a The Gabriele Group, LLC) based upon agreements signed July 31, 2002. Legal expenses for patents increased from approximately $215,000 in 2003 to approximately $481,000 in 2004. Legal fees increased from approximately $650,000 in 2003 to approximately $1,610,000 in 2004 primarily due to increased litigation fees. Expenses relating to the start-up and consolidation of Immtech Therapeutics and Immtech Hong Kong into Immtech accounts were approximately $398,000. Accounting fees increased from approximately $125,000 in 2003 to approximately $231,000 in 2004. Additionally, the -59- expensing of a retainer fee to Wyndham increased general and administrative expenses in 2004 by $160,000. We incurred a net loss of approximately $12,866,000 for the year ended March 31, 2004, as compared to a net loss of approximately $4,679,000 for the year ended March 31, 2003. In 2004, we also charged deficit accumulated during the development stage of approximately $3,526,000 of non-cash convertible preferred stock dividends and convertible preferred stock premium deemed dividends. Year Ended March 31, 2003 Compared with Year Ended March 31, 2002 Revenues under collaborative research and development agreements were approximately $1,609,000 and $3,522,000 in the years ended March 31, 2003 and 2002, respectively. In 2003, we recognized revenues of approximately $1,389,000 relating to a clinical research subcontract agreement with UNC funded by a grant that UNC received from The Gates Foundation, compared to approximately $2,946,000 in 2002. We also recognized approximately $70,000 from SBIR grants in 2003, while in 2002 there were grant revenues of approximately $576,000 through STTR and SBIR programs from the NIH. Research and development expenses decreased from approximately $2,570,000 in 2002 to $3,958,000 in 2003. The decrease in research and development costs is primarily attributable to the decrease in the revenues relating to the clinical research subcontract agreement with UNC and the decrease in the grant revenues from SBIR grants from the NIH. General and administrative expenses were approximately $3,732,000 in 2003, compared to approximately $2,928,000 in 2002. In the year ended 2003, there were general and administrative compensation expenses of approximately $758,000 related to the issuance of 150,000 shares of common stock to Cheung Ming Tak to act as our non-exclusive agent to develop and qualify potential strategic partners for the purpose of testing and/or commercializing Company products in the PRC. We incurred a net loss of approximately $4,679,000,000 for the year ended March 31, 2003, as compared to a net loss of approximately $3,323,0000 for the year ended March 31, 2003. In 2002 and 2003, respectively, we also charged deficit accumulated during the development stage of approximately $938,000 and $452,000 of non-cash convertible preferred stock dividends. Impact of Inflation Although it is difficult to predict the impact of inflation on our costs and revenues in connection with our operations, we do not anticipate that inflation will materially impact our costs of operation or the profitability of our products when and if marketed. -60- Unaudited Selected Quarterly Information The following table sets forth certain unaudited selected quarterly information (amounts in thousands, except per share amounts): -61- Fiscal Quarter Ended ------------------------------------------------------------------------------------------------- ------------------------------------------------- ------------------------------------------- December September December September March 31, 31, 30, June 30, March 31, 31, 30, June 30, 2004 2003 2003 2003 2003 2002 2002 2002 --------- -------- --------- -------- -------- -------- -------- -------- Statements of Operations Data: REVENUES ...................... $ 618 $ 654 $ 659 $ 485 $ 585 $ 234 $ 360 $ 430 EXPENSES: Research and development ................ 966 815 905 607 706 402 711 751 General and administrative .. 1,807(7) 2,580(6) 6,596(5) 1,007(4) 673 724 883(3) 1,452(2) ------- ------- ------- ------- ------- ------- ------- ------- Total expenses ......... 2,773 3,395 7,501 1,614 1,379 1,126 1,594 2,203 ------- ------- ------- ------- ------- ------- ------- ------- LOSS FROM OPERATIONS .......... (2,155) (2,741) (6,842) (1,129) (794) (892) (1,234) (1,773) OTHER INCOME(EXPENSE): Interest income ............. 10 6 4 1 1 3 2 8 ------- ------- ------- ------- ------- ------- ------- ------- NET LOSS ...................... (2,145) (2,735) (6,838) (1,128) (793) (889) (1,232) (1,765) CONVERTIBLE PREFERRED STOCK DIVIDENDS AND PREFERRED STOCK PREMIUM DEEMED DIVIDENDS(1) ......... (2,107) (131) (93) (1,195) (89) (96) (207) (60) ------- ------- ------- ------- ------- ------- ------- ------- NET LOSS ATTRIBUTABLE TO COMMON STOCKHOLDERS ................ $(4,252) $(2,866) $(6,931) $(2,323) $ (882) $ (985) $(1,439) $(1,825) ======= ======= ======= ======= ======= ======= ======= ======= NET LOSS PER SHARE ATTRIBUTABLE TO COMMON STOCKHOLDERS: Net loss ...................... $ (0.22) $ (0.30) $ (0.79) $ (0.14) $ (0.11) $ (0.14) $ (0.20) $ (0.29) Convertible preferred stock dividends and convertible preferred stock premium deemed dividends ............ $ (0.22) $ (0.01) $ (0.01) $ (0.15) $ (0.01) $ (0.02) (0.03) (0.01) ------- ------- ------- ------- ------- ------- ------- ------- BASIC AND DILUTED NET LOSS PER SHARE ATTRIBUTABLE TO COMMON STOCKHOLDERS ................ $ (0.44) $ (0.31) $ (0.80) $ (0.29) $ (0.12) $ (0.16) $ (0.23) $ (0.30) ======= ======= ======= ======= ======= ======= ======= ======= -62- (1) See Note 7 to Notes to Financial Statements for a discussion on the convertible preferred stock dividends. (2) Includes $758 of costs related to the issuance of 150,000 shares of common stock to Cheung Ming Tak to act as our non-exclusive agent to develop and qualify potential strategic partners for the purpose of testing and/or the commercialization of Company products in the PRC. (3) Includes $188 of costs related to the issuance of 40,000 shares of common stock to The Gabriele Group, L.L.C. for assistance with respect to management consulting, strategic planning, public relations and promotions. (4) Includes $337 of costs related to the issuance of 25,000 common shares and the vesting of 87,500 warrants to Fulcrum under the agreement signed March 21, 2003. (5) Includes (i) $2,744 of costs related to the issuance of warrants to purchase 600,000 shares of common stock issued to China Harvest International Ltd. as payment for services to assist in obtaining regulatory approval to conduct clinical trials in China, (ii) $63 for the issuance of 10,000 shares of common stock issued to Mr. David Tat Koon Shu for consulting services in China, (iii) $1,400 for the issuance of 100,000 shares of common stock issued to Fulcrum for assisting with listing our securities on a recognized stock exchange and for consulting services, and (iv) $1,016 for the issuance of 25,000 common shares and the vesting of 87,500 warrants to Fulcrum under the agreement signed March 21, 2003. (6) Includes (i) $947 of costs related to the issuance of 25,000 common shares and the vesting of 87,500 warrants to Fulcrum under the agreement signed March 21, 2003, and (ii) $247 for the attainment of certain milestones with respect to the vesting of warrants to purchase 20,000 shares of common stock issued to Pilot Capital Group, LLC (f/k/a The Gabriele Group, LLC) based upon agreements signed July 31, 2002. (7) Includes $480 of costs related to the issuance of 16,667 common shares and the vesting of 58,335 warrants to Fulcrum under the agreement signed March 21, 2003. -63- ITEM 7A. QUANTITATIVE AND QUALITATIVE DISCLOSURES ABOUT MARKET RISK The exposure of market risk associated with risk-sensitive instruments is not material, as our operations are conducted primarily in U.S. dollars and we invest primarily in short-term government obligations and other cash equivalents. We intend to develop policies and procedures to manage market risk in the future if and when circumstances require. ITEM 8. FINANCIAL STATEMENTS AND SUPPLEMENTARY DATA Our financial statements appear following Item 15 of this report and are incorporated herein by reference. ITEM 9. CHANGES IN AND DISAGREEMENTS WITH ACCOUNTANTS ON ACCOUNTING AND FINANCIAL DISCLOSURE None. ITEM 9A CONTROLS AND PROCEDURES Disclosures and Procedures We maintain controls and procedures designed to ensure that we are able to collect the information we are required to disclose in the reports we file with the SEC, and to process, summarize and disclose this information within the time periods specified in the rules of the SEC. Our Chief Executive and Chief Financial Officers are responsible for establishing and maintaining these procedures and, as required by the rules of the SEC, evaluate their effectiveness. Based on their evaluation of our disclosure controls and procedures, which took place as of the end of the period covered by this Annual Report on Form 10-K, our Chief Executive and Chief Financial Officers believe that these procedures are effective to ensure that we are able to collect, process and disclose the information we are required to disclose in the reports we file with the SEC within the required time periods. Internal Controls We maintain a system of internal controls designed to provide reasonable assurance that: transactions are executed in accordance with management's general or specific authorization; transactions are recorded as necessary (i) to permit preparation of financial statements in conformity with generally accepted accounting principles and (ii) to maintain accountability for assets. Access to assets is permitted only in accordance with management's general or specific authorization and the recorded accountability for assets is compared with the existing assets at reasonable intervals and appropriate action is taken with respect to any differences. Since the date of the most recent evaluation of our internal controls by our Chief Executive and Chief Financial Officers, there have been no significant changes in such controls -64- or in other factors that could have significantly affected those controls, including any corrective actions with regard to significant deficiencies and material weaknesses. PART III. ITEM 10. DIRECTORS AND EXECUTIVE OFFICERS OF THE REGISTRANT Information Regarding Directors and Executive Officers The table below sets forth the names and ages of our directors and executive officers as of June 4, 2004, as well as the positions and offices held by such persons. A summary of the background and experience of each of these individuals is set forth after the table. Each director serves for a term of one year and is eligible for reelection at our next annual shareholders' meeting. Name Age Position(s) ------------------------ ---- ------------------------------------------------ T. Stephen Thompson 57 Director, President and Chief Executive Officer Cecilia Chan 41 Director and Executive Vice President Gary C. Parks 54 Treasurer, Secretary and Chief Financial Officer Harvey R. Colten, MD 65 Director Judy Lau 44 Director Levi H.K. Lee, MD 63 Director Eric L. Sorkin 44 Director Frederick W. Wackerle 65 Director T. Stephen Thompson, President, Chief Executive Officer and Director. Mr. Thompson has served as a Director since November 27, 1991. He joined Immtech in April 1991 from Amersham Corporation, where he was President and Chief Executive Officer. He was responsible for Amersham Corporation's four North American divisions: Life Sciences, Radiopharmaceuticals, Diagnostics and Quality and Safety Products. In addition, he had direct responsibility for the Clinical Reagent (in vitro diagnostic) Division in the United Kingdom. He was employed by Amersham Corporation from 1986 to 1991. Mr. Thompson has 20 years' experience in healthcare, with previous positions as President of a small diagnostic start-up, General Manager of the Infectious Disease and Immunology Business Unit in the Diagnostic Division of Abbott Laboratories from 1981 to 1986, and Group Marketing Manager for the Hyland Division of Baxter International Inc. from 1978 to 1981. Mr. Thompson is a member of -65- the Board of Directors of Matritech, Inc. (NASDAQ: NMPS). Mr. Thompson holds a B.S. from the University of Cincinnati and an MBA from Harvard University. Cecilia Chan, Executive Vice President and Director. Ms. Chan has served as Director since November 16, 2001. She has 18 years of experience in making investments and business development. She began working on Immtech's growth strategy in 1998 as a private investor, spearheading Immtech's initial public offering in April 1999. She joined Immtech as Vice President in July, 1999 and was elected to our board of directors in November 2001. Ms. Chan is responsible for strategic development, creating joint ventures and licensing agreements, fund raising and directing our uses of capital resources as we advances through milestones and various growth stages. Prior to joining Immtech, Ms. Chan was a Vice President at Dean Witter Realty, Inc. until 1993 and thereafter concentrated her efforts as a private investor until she joined Immtech. During her eight years at Dean Witter, Ms. Chan completed over $500 million in investments and was vice-president of public partnerships having assets in excess of $800 million. Since 1993, Ms. Chan has developed and funded investments in the United States and the PRC. She graduated from New York University in 1985 with a Bachelor of Science degree in International Business. Judy Lau, Director. Ms. Lau has served as Director since October 31, 2003. Since July 2002 to date, Ms. Lau has served as the Chairperson of Convergent Business Group, a Hong Kong-based investment advisory firm with investments focused in high technology, life sciences, healthcare and environmental engineering projects in the greater China region. From May of 2001 to July of 2002, Ms. Lau served as General Manager of China Overseas Venture Capital Co. Ltd., a venture capital firm. From October of 2000 to April of 2001, Ms. Lau served as Chief Executive Officer of the Good Fellow Group, a Chinese investment firm; and from March of 1999 to September of 2000, Ms. Lau was the Managing Director of America Online HK, an Internet Service Provider and Hong Kong affiliate of Time Warner, Inc. From April of 1998 to February of 1999, Ms. Lau worked as a consultant to Pacific Century Group. Ms. Lau has served in the position of Director of Immtech Hong Kong Ltd. since June, 2003. Ms. Lau was named in 2000, one of the thirty-six most influential Business Women of Hong Kong by Capital Magazine and is a Fellow of the Hong Kong Association for the Advancement of Science and Technology. Levi Hong Kaye Lee, M.D., Director. Dr. Lee has served as Director since October 31, 2003. Dr. Lee has been in private medical practice, specializing in pediatrics, since 1971. His practice is located in Hong Kong. Dr. Lee received a B.A. in Biochemistry from the University of California, Berkeley, in 1962, and received his M.D. from the University of California, San Francisco, in 1966. Dr. Lee has served in the position of Director of Immtech Hong Kong Ltd. since June, 2003. He was appointed a Diplomat of the American Board of Pediatrics in 1971. Gary C. Parks, Treasurer, Secretary and Chief Financial Officer. Mr. Parks joined Immtech in January 1994, having previously served at Smallbone, Inc., from 1989 until 1993, where he was Vice President, Finance. Mr. Parks was a Division Controller with International Paper from 1986 to 1989. Prior to that, he was Vice President, Finance, of SerckBaker, Inc., a subsidiary of BTR plc, from 1982 to 1986 and a board member of -66- SerckBaker de Venezuela. Mr. Parks holds a B.A. from Principia College and an MBA from the University of Michigan. Harvey Colten, MD, Director. Dr. Colten has served as Director since October 30, 2000. He is currently Vice President and Senior Associate Dean for Academic Affairs at Columbia University Health Sciences Division and College of Physicians and Surgeons. Prior to this, he served as Chief Medical Officer at iMetrikus, Inc., a healthcare Internet company focused on improving the communication between the patient, physician and the medical industry from 2000 until 2002, and prior to that he was the Dean of the Medical School and Vice President for Medical Affairs at Northwestern University from 1997 to 2000. He previously served as the Harriet B. Spoehrer Professor and Chair of the Department of Pediatrics and Professor of Molecular Microbiology at Washington University School of Medicine, St. Louis, Missouri, whose faculty he joined in 1986. He earned a B.A. at Cornell University in 1959, an MD from Western Reserve University in 1963, and an M.A. (honorary) from Harvard in 1978. Following his clinical training, he was a researcher at the National Institutes of Health from 1965 to 1970. In 1970, he was appointed to the faculty at the Harvard Medical School, where he was named Professor of Pediatrics in 1979 and Chief of the Division of Cell Biology, Pulmonary Medicine, and Director of the Cystic Fibrosis Program at Children's Hospital Medical Center, Boston. He is a member of the Institute of Medicine and was Vice-Chair of its Council. He is a member of the American Society for Clinical Investigation, the Society for Pediatric Research, the Association of American Physicians, the American Pediatric Society, the American Association of Immunologists (former secretary and treasurer), and the American Society for Biochemistry and Molecular Biology. He is also a Fellow of the American Association for the Advancement of Science, the American Academy of Allergy and Immunology and the American Academy of Pediatrics. Dr. Colten is a Diplomat of the American Board of Pediatrics, served on the American Board of Allergy and Immunology, was a member of the National Heart, Lung, and Blood Institute Advisory Council, and serves on the Board of Directors of the Oasis Institute and the March of Dimes Scientific Advisory Council, in addition to many other Federal and private health groups that advise on scientific and policy issues. Dr. Colten also served as Vice Chairman of the Board of Directors of Parents as Teachers National Center. He has been on editorial boards and advisory committees of several leading scientific and medical journals, including the New England Journal of Medicine, Journal of Clinical Investigation, Journal of Pediatrics, Journal of Immunology, Annual Review of Immunology, Proceedings of the Association of American Physicians and American Journal of Respiratory Cell and Molecular Biology. Eric L. Sorkin, Director. Mr. Sorkin has served as Director since January 6, 2000. He is a private investor. Prior to 1994, Mr. Sorkin worked for eleven years at Dean Witter Realty Inc., a wholly owned subsidiary of Morgan Stanley, which grew to hold an investment portfolio of real estate and other assets of over $3 billion. He became a Managing Director in 1988 and was responsible for the acquisition, structuring and debt placement of various investments including real estate, fund management and asset-backed securities. Mr. Sorkin managed Dean Witter Realty's retail (shopping center) portfolio of over two million square feet, and participated in the development of office, residential, industrial and retail property and in the acquisition of over five million square feet of properties. Since 1994, Mr. Sorkin has developed and funded investments in the United States and the PRC. He is a graduate of Yale University with a Bachelor of Arts degree in Economics. -67- Frederick W. Wackerle, Director. Mr. Wackerle has served as Director since December 17, 2001. He is an author, private investor and President of Fred Wackerle, Inc. He has been an advisor to Chief Executive Officers ("CEOs") and boards and previously was an executive search consultant for 35 years. Mr. Wackerle specialized in advising corporate boards on management succession. In the past ten years, he devoted a significant amount of his time to investing in and advising biotechnology companies on succession planning, and recruited CEO candidates and board members for companies that include Biogen, Inc., ICOS Corp., Amylin Pharmaceuticals, Inc., Enzon, Inc., Medtronic Inc. and Ventana Medical Systems. Mr. Wackerle has recently published a book on management succession entitled, "The Right CEO-Straight Talk About Making CEO Selection Decisions" (Jossey-Bass), and is a graduate of Monmouth College, Illinois, where he has been active on their Board of Trustees. He is also a board member of The Rehabilitation Institute of Chicago. Section 16(a) Beneficial Ownership Reporting Compliance Section 16(a) of the Exchange Act requires our directors, executive officers and 10% stockholders of a registered class of equity securities to file reports of ownership and reports of changes in ownership of our common stock and other equity securities with the SEC. Directors, executive officers and 10% stockholders are required to furnish us with copies of all Section 16(a) forms they file. Based on a review of the copies of such reports furnished to us, we believe that during fiscal 2003, our directors, executive officers and 10% stockholders complied with all Section 16(a) filing requirements applicable to them. Ms. Vivian Lee, the wife of Dr. Lee, one of our independent directors, purchased 2,000 shares and sold 1,000 shares of our common stock in a series of trades on February 5, 2004, resulting in a profit of $235 to Ms. Lee. Dr. Lee paid $235 to us as a Section 16 fee. Board Committees The board of directors has an audit committee, a compensation committee and a nominating committee. The function, composition, and number of meetings of each of these committees are described below. Audit Committee The audit committee (a) has sole authority to appoint, replace and compensate our independent auditors and is directly responsible for oversight of their work; (b) approves all audit fees and terms, as well as any permitted non-audit services; (c) meets and discusses directly with our independent auditors their audit work and related matters and (d) oversees and performs such investigations with respect to our internal and external auditing procedures and affairs as the audit committee deems necessary or advisable and as may be required by applicable law. The members of the audit committee are Directors Sorkin (Chairman), Colten and Lau. Each member of the audit committee is "independent" in accordance with the rules of the SEC and the listing standards of the American Stock Exchange. The board has determined that Mr. Eric Sorkin, the current chairman of the audit committee, qualifies as an "audit committee financial expert" within the meaning of the regulations of the SEC. -68- Compensation Committee The compensation committee (a) annually reviews and determines salaries, bonuses and other forms of compensation paid to our executive officers and management; (b) selects recipients of awards of incentive stock options and non-qualified stock options and establishes the number of shares and other terms applicable to such awards; and (c) construes the provisions of and generally administers the First Amended and Restated Immtech International, Inc. 2000 Stock Incentive Plan. The members of the compensation committee are Directors Wackerle (Chairman), Lau and Sorkin. Nominating Committee The nominating committee has authority to review the qualifications of, interview and nominate candidates for election to the board of directors. The members of the nominating committee are Directors Colten (Chairman), Lee and Wackerle. Each member of the nominating committee is "independent" in accordance with the listing standards of the American Stock Exchange. Code of Ethics We have adopted a "code of ethics", as defined by the SEC, that applies to our Chief Executive Officer, Chief Financial Officer, principal accounting officer and persons performing similar functions with Immtech and our subsidiaries. We have filed with the SEC a copy of our Code of Ethics as Exhibit 14.1 to this Annual Report on Form 10-K. We also post the text of our Code of Ethics on our Internet website (www.immtech-international.com). ITEM 11. EXECUTIVE COMPENSATION Summary Compensation Table The following table sets forth certain information regarding the compensation of our Chief Executive Officer, our Executive Vice President and our Chief Financial Officer for the fiscal years ended March 31, 2002, 2003 and 2004. Except as set forth below, no other compensation was paid to these individuals during the years indicated. -69- Long-Term Annual Compensation Compensation Awards ------------ ---------------- Securities Underlying Year Salary ($) Options/SARs (#) ---- ----------- ---------------- T. Stephen Thompson 2004 $185,000 40,000 President, Chief Executive Officer 2003 $150,000 75,000 and Director 2002 $150,000 0 Cecilia Chan 2004 $148,000 25,000 Executive Vice President and 2003 $120,000 50,000 Director 2002 $120,000 0 Gary C. Parks 2004 $134,375 15,000 Secretary, Treasurer and Chief 2003 $143,250(1) 25,000 Financial Officer 2002 $125,000 10,000 ------------ (1) Includes a bonus of $18,250. Stock Option Grants and Exercises During the Fiscal Year Ended March 31, 2004 The following table sets forth information concerning stock option grants made during the fiscal year ended March 31, 2004, to our executive officers named in the "Summary Compensation Table" above. This information is for illustration purposes only and is not intended to predict the future price of our common stock. The actual future value of the options will depend on the market value of the common stock. STOCK OPTION GRANTS IN FISCAL YEAR ENDED MARCH 31, 2004 Potential Realizable Value At Assumed Annual Rates of Stock Individual Grants Price Appreciation For Option Term ---------------------------------------------------------------------------------- ----------------------------------- Percent of Total Number of Options/SARs Securities Granted Underlying to Exercise Options/SARs Employees Price Expiration Name Granted (%) ($/SH) Date 5%($) 10%($) ------------------------- ------------ ------------- --------- ----------- --------- ---------- T. Stephen Thompson 40,000 30.30 21.66 11/5/2013 1,411,274 2,247,218 Cecilia Chan 25,000 18.94 21.66 11/5/2013 882.046 1,404,512 Gary C. Parks 15,000 11.36 21.66 11/5/2013 529,228 842,707 -70- The following table sets forth certain summary information concerning exercised and unexercised options and warrants to purchase common stock held by the executive officers named in the "Summary Compensation Table" as of March 31, 2004. STOCK OPTION AND WARRANT EXERCISES IN FISCAL YEAR ENDED MARCH 31, 2004, AND FISCAL YEAR-END OPTION/WARRANT VALUES Number of Unexercised Value of Unexercised Options/Warrants at Fiscal In-The-Money Options/Warrants Shares Year End (#) at Fiscal Year End ($) Acquired on Realized ----------------------------- --------------------------------- Exercise (#) Value ($) Exercisable Unexercisable Exercisable Unexercisable ------------ --------- ----------- ------------- ------------- ------------- T. Stephen Thompson 0 0 87,653 75,414 1,209,630(1) 698,640(2) Cecilia Chan 0 0 253,355 48,957 3,072,060(3) 465,765(4) Gary C. Parks 0 0 37,628 27,567 492,703(5) 242,284(6) -------------------------------------------------------------------------------------------------------------------------------- ------------ (1) Based on the March 31, 2004, value of $18.52 per share, minus the average per share exercise price of $3.27 multiplied by the number of shares underlying the options and warrants. (2) Based on the March 31, 2004, value of $18.52 per share, minus the average per share exercise price of $2.55 multiplied by the number of shares underlying the options. (3) Based on the March 31, 2004, value of $18.52 per share, minus the average per share exercise price of $6.14 multiplied by the number of shares underlying the options and warrants. (4) Based on the March 31, 2004, value of $18.52 per share, minus the average per share exercise price of $2.55 multiplied by the number of shares underlying the options. (5) Based on the March 31, 2004, value of $18.52 per share, minus the average per share exercise price of $4.24 multiplied by the number of shares underlying the options and warrants. (6) Based on the March 31, 2004, value of $18.52 per share, minus the average per share exercise price of $3.08 multiplied by the number of shares underlying the options. Director Compensation We compensate non-employee members of the Board of Directors for their service as Board members through the grant to each such director of 20,000 options to purchase our common stock upon joining the Board. In addition, each non-employee director receives options to purchase 15,000 shares of common stock for each subsequent year of Board service, options to purchase 3,000 shares of common stock for each year of service on each Board committee and options to purchase 1,000 shares of common stock for each Board committee chaired. Such options are generally granted at fair market value on the date of grant, vest ratably over 2 years and expire 10 years from the date of grant. We also reimburse the directors for out-of-pocket expenses incurred in connection with their service as directors. -71- Employment Agreements We entered into an employment agreement with T. Stephen Thompson in 1992, pursuant to which we retained Mr. Thompson as our President and Chief Executive Officer for an annual base salary of $150,000 (subject to annual adjustment by the Board), plus reimbursement for related business expenses. The agreement, which includes certain confidentiality and non-disclosure provisions, grants to Mr. Thompson the right to receive an annual bonus to be established by the Board in an amount not to exceed 60% of Mr. Thompson's annual base salary for the year and certain other fringe benefits. If we breach the agreement or Mr. Thompson is terminated by us without cause, he is entitled to all payments which he would otherwise accrue over the greater of nine months from the date of termination or the remaining term under the agreement. Additionally, rights to all options granted to Mr. Thompson pursuant to the agreement vest immediately upon his termination without cause or a change of control. The term of Mr. Thompson's agreement expired on May 11, 1999; however, the agreement is subject to automatic renewal for successive one-year terms unless terminated by either party upon 30 days' notice. Except for $12,500 paid to Mr. Thompson during the fiscal year ended March 31, 1998, Mr. Thompson has waived any right to receive salary due under his employment agreement prior to June 30, 1998. Beginning July 1, 1998, and continuing until April 30, 1999, Mr. Thompson agreed to accept one-half of his annual salary as full satisfaction of our salary obligation under his employment agreement. Mr. Thompson, effective May 1, 1999, has resumed his full salary rate of $150,000 per annum under his employment agreement, but will not be paid amounts previously waived. Effective September 1, 2003, Mr. Thompson received a raise to $210,000 per year. Compensation Committee Interlocks and Insider Participation No interlocking relationship exists between our Board of Directors or our Compensation Committee and the board of directors or compensation committee of any other company, nor has any such interlocking relationship existed in the past. ITEM 12. SECURITY OWNERSHIP OF CERTAIN BENEFICIAL OWNERS AND MANAGEMENT The following table sets forth certain information regarding the beneficial ownership of our common stock as of June 4, 2004, by (i) each of our directors and executive officers, (ii) all directors and executive officers as a group and (iii) each person known to be the beneficial owner of more than 5% of our common stock. Number of Shares Percentage of Outstanding of Common Stock Beneficially Shares Name and Address Owned of Common Stock ------------------------------------------------------- ------------------------------- ----------------------------- T. Stephen Thompson (1) c/o Immtech International, Inc. 150 Fairway Drive, Ste. 150 Vernon Hills, IL 60061 444,842 shares 4.42% -72- Number of Shares Percentage of Outstanding of Common Stock Beneficially Shares Name and Address Owned of Common Stock ------------------------------------------------------- ------------------------------- ----------------------------- Cecilia Chan (2) c/o Immtech International, Inc. One North End Ave. New York, NY 10282 303,201 shares 2.98% Gary C. Parks (3) c/o Immtech International, Inc. 150 Fairway Drive, Ste. 150 Vernon Hills, IL 60061 68,070 shares 0.68% Harvey Colten, M.D. (4) c/o Office of the Dean Columbia University College of Physicians and Surgeons 630 West 168th Street New York, NY 10032 36,311 shares 0.37% Judy Lau (5) Unit 2905, Shui On Centre 6-8 Harbour Road Wanchai, Hong Kong 12,750 shares 0.13% Levi H.K. Lee, M.D.(6) 1405 Lane Crawford House 70 Queens Road Central, Hong Kong 209,127 shares 2.10% Eric L. Sorkin (7) c/o Immtech International, Inc. One North End Ave. New York, NY 10282 313,229 shares 3.07% Frederick W. Wackerle(8) 3750 N. Lake Shore Drive Chicago IL 60613 75,902 shares 0.76% -73- Number of Shares Percentage of Outstanding of Common Stock Beneficially Shares Name and Address Owned of Common Stock ------------------------------------------------------- ------------------------------- ----------------------------- All executive officers and directors as a group (8 persons) 1,463,432 shares 13.48% Chan Kon Fung Flat B, 16th Floor 132 Broadway Mei Foo Sun Chuen Kowloon, Hong Kong 1,246,600 shares 12.59% ------------ (1) Includes (i) 284,439 shares of common stock; (ii) 45,249 shares of common stock issuable upon the conversion of series A preferred stock; (iii) 12,500 shares of common stock issuable upon the conversion of series B preferred stock; (iv) 25,000 shares of common stock issuable upon the exercise of warrants as follows: warrant to purchase 20,000 shares of common stock at $6.00 per share by February 14, 2007 (only after the series A preferred stock has been converted and vested), and warrant to purchase 5,000 shares of common stock at $6.125 per share by September 25, 2007; and (v) 77,654 shares of common stock issuable upon the exercise of options as follows: vested option to purchase 8,872 shares of common stock at $0.46 per share by March 21, 2006, vested option to purchase 14,195 shares of common stock at $1.74 per share by April 16, 2008, the vested portion of 39,587 shares of an option to purchase 75,000 shares of common stock at $2.55 per share by December 24, 2012, and the vested portion of 15,000 shares of an option to purchase 40,000 shares of common stock at $21.66 per share by November 5, 2013. (2) Includes (i) 34,342 shares of common stock; (ii) 5,781 shares of common stock issuable upon the conversion of series B preferred stock; (iii) 227,312 shares of common stock issuable upon the exercise of warrants as follows: vested warrant to purchase 51,923 shares of common stock at $6.47 per share by July 24, 2004, vested warrant to purchase 173,077 shares of common stock at $6.47 per share by October 12, 2004, and vested warrant to purchase 2,312 shares of common stock at $6.125 per share by September 25, 2007; and (iv) 35,766 shares of common stock issuable upon the exercise of options as follows: the vested portion of 26,391 shares of an option to purchase 50,000 shares of common stock at $2.55 per share by December 24, 2012, and the vested portion of 9,375 shares of an option to purchase 25,000 shares of common stock at $21.66 per share by November 5, 2013. (3) Includes (i) 21,792 shares of common stock; (ii) 2,262 shares of common stock issuable upon the conversion of series A preferred stock; (iii) 1,000 shares of common stock issuable upon the exercise of warrants as follows: warrant to purchase 1,000 shares of common stock at $6.00 per share by February 14, 2007 (only after the series A preferred stock has been converted); and (iv) 43,016 shares of common stock issuable upon the exercise of options as follows: vested option to purchase 14,195 shares of common stock at $1.74 per share by April 16, 2008, vested option to purchase 10,000 shares of common stock at $10.00 per share by July 19, 2011, the vested portion of 13,196 shares of an option to purchase 25,000 shares of common stock at $2.55 per share by December 24, 2012, and the vested portion of 5,625 shares of an option to purchase 15,000 shares of common stock at $21.66 per share by November 5, 2013. (4) Includes (i) 1,088 shares of common stock; and (ii) 35,223 shares of common stock issuable upon the exercise of options as follows: vested option to purchase 20,000 shares of common stock at $10.50 per shares by December 28, 2005, the vested portion of 6,028 shares of an option to purchase 7,000 shares of common stock at $4.75 per share by December 18, 2006, the vested portion of 3,695 shares of an option to purchase 7,000 shares of common stock at $2.55 per share by December 24, 2007, and the vested portion of 5,500 shares of an option to purchase 22,000 shares of common stock at $14.29 per share by February 1, 2014. (5) Includes 12,750 shares of common stock issuable upon the exercise of options as follows: the vested portion of 7,500 shares of an option to purchase 20,000 shares of common stock at $21.66 per share by November 5, 2013, -74- and the vested portion of 5,250 shares of an option to purchase 21,000 shares of common stock at $14.29 per share by February 1, 2014. (6) Includes (i) 133,778 shares of common stock; (ii) 11,312 shares of common stock issuable upon the conversion of series A preferred stock; (iii) 52,037 shares of common stock issuable upon the conversion of series C preferred stock; and (iv) 12,000 shares of common stock issuable upon the exercise of options as follows: the vested portion of 7,500 shares of an option to purchase 20,000 shares of common stock at $21.66 per share by November 5, 2013, and the vested portion of 4,500 shares of an option to purchase 18,000 shares of common stock at $14.29 per share by February 1, 2014. (7) Includes (i) 26,420 shares of common stock; (ii) 20,362 shares of common stock issuable upon the conversion of series A preferred stock; (iii) 234,000 shares of common stock issuable upon the exercise of warrants as follows: vested warrant to purchase 51, 923 shares of common stock at $6.47 per share by July 24, 2004, vested warrant to purchase 173,077 shares of common stock at $6.47 per share by October 12, 2004, and vested warrant to purchase 9,000 shares of common stock at $6.00 per share by February 14, 2007 (only after the series A preferred stock has been converted); and (iv) 32,447 shares of common stock issuable upon the exercise of options as follows: the vested portion of 23,252 shares of an option to purchase 27,000 shares of common stock at $4.75 per share by December 18, 2006, the vested portion of 3,695 shares of an option to purchase 7,000 shares of common stock at $2.55 per share by December 24, 2007, and the vested portion of 5,500 shares of any option to purchase 22,000 shares of common stock at $14.29 per share by February 1, 2014. (8) Includes (i) 13,186 shares of common stock; (ii) 13,575 shares of common stock issuable upon the conversion of series A preferred stock; (iii) vested warrant to purchase 6,000 shares of common stock at $6.00 per share by February 14, 2007 (only after the series A preferred stock has been converted); and (iv) 43,141 shares of common stock issuable upon the exercise of options as follows: the vested option to purchase 15,000 shares of common stock at $10.50 per share by December 28, 2005, the vested portion of 18,946 shares of an option to purchase 22,000 shares of common stock at $4.75 per share by December 18, 2006, the vested portion of 3,695 on an option to purchase 7,000 shares of common stock at $2.55 per share by December 24, 2007, and the vested portion of 5,500 shares of an option to purchase 22,000 shares of common stock at $14.29 per share by February 1, 2014. ITEM 13. CERTAIN RELATIONSHIPS AND RELATED TRANSACTIONS The following related-party transactions are disclosed. RADE Management Corporation --------------------------- From January 1998 to July 1999 we utilized the services of RADE Management Corporation ("RADE") as a consultant to assist us to raise capital and to assist us with our initial public offering. On July 1, 1999, Immtech began leasing office space from RADE in RADE's facility in New York, New York on a month-to-month basis to house our business development, investor relations and certain of our administrative functions. During the years ended March 31, 2002, 2003 and 2004, we paid approximately $106,000, $106,000 and $121,000, respectively, for the use of the facility. In addition, during the years ended March 31, 2002, 2003 and 2004, we reimbursed RADE approximately $18,000, $0 and $0, respectively, for expenses paid on our behalf. We have researched leasing other facilities in the New York metropolitan area and believe that our Lease with RADE is on terms no less favorable than we would otherwise obtain from another unaffiliated third-party. -75- Super Insight Limited --------------------- On November 28, 2003, we entered into a share purchase agreement and deed of indemnity related to the purchase of Super Insight Limited (the "Share Purchase Agreement") and an Allonge to the Share Purchase Agreement related to the shares in Super Insight Limited ("Super Insight") and Immtech Hong Kong Limited ("Immtech Hong Kong") (the "Allonge") with Mr. Chan Kon Fung ("Mr. Chan"), Lenton Fibre Optics Development Limited, Super Insight and Immtech Hong Kong. Pursuant to the terms of the Share Purchase Agreement and the Allonge, we purchased (i) from Mr. Chan 100% of the outstanding shares of Super Insight and its wholly-owned subsidiary, subsequently named Immtech Life Science Limited ("Immtech Life Science") and (ii) from Lenton, 100% of Lenton's interest in Immtech Hong Kong. As payment for Super Insight and Immtech Hong Kong, we transferred to Mr. Chan our 80% interest in Lenton and paid him $400,000 in cash In November 2002, Mr. Chan Kon Fung, the counterparty in the Super Insight transaction listed above, received 1,200,000 shares of our common stock in exchange for an 80% interest in Lenton Fibre Optics Development Limited; the same 80% interest we are transferring to Mr. Chan to obtain the 100% interest in Super Insight. With 1,200,000 shares of our common stock, Mr. Chan became and remains, a "10% beneficial owner" of Immtech and therefor our board determined that the acquisition of Super Insight required increased scrutiny as an affiliate transaction. Our board reviewed the Super Insight transaction prior to its completion and determined that the terms of the transaction were no less favorable to us than we could have obtained in a similar transaction with an unaffiliated third party and therefore approved the transaction. ITEM 14. PRINCIPAL ACCOUNTANT FEES AND SERVICES The following table presents the aggregate fees billed for professional services rendered by Deloitte & Touche LLP during the years ended March 31, 2003 and 2004. Other than as set forth below, no professional services were rendered or fees billed by Deloitte & Touche LLP during 2003 or 2004. 2004 2003 Audit Fees (a) $ 205,000 $ 113,000 Audit Related Fees -- -- --------- --------- Total Audit and Audit Related Fees 205,000 113,000 Tax Fees (b) 4,000 4,000 All Other Fees -- -- --------- --------- Total Fees $ 209,000 $ 117,000 ========= ========= (a) Includes fees and out-of-pocket expenses for the following services: Audit of the consolidated financial statements Quarterly reviews SEC filings and consents Financial accounting and reporting consultations (Lenton, Super Insight and Others) (b) Includes fees and out-of-pocket expenses for tax compliance, tax planning and advice. All work performed by Deloitte & Touche as described above has been approved by the Audit Committee -76- prior to Deloitte & Touche's engagement to perform the audit. The Audit Committee pre-approves on an annual basis the audit, audit-related, tax and other services to be rendered by our accountants based on historical information and anticipated requirements for the following fiscal year. To the extent that our management believes that a new service or the expansion of a current service provided by our accountants is necessary, such new or expanded service is presented to the Audit Committee or one of its members for review and approval. PART IV ITEM 15. EXHIBITS, FINANCIAL STATEMENT SCHEDULES AND REPORTS ON FORM 8-K (a) Documents Filed with this Report. The following documents are filed as part of this Form 10-K: 1. Financial Statements The consolidated financial statements required by this item are submitted in a separate section beginning on page F-1 of this report. 2. Financial Statement Schedules None. 3. Exhibits The information called for by this paragraph is contained in the Index to Exhibits of this Form 10-K, which is incorporated herein by reference. (b) Reports on Form 8-K. On December 2, 2003, we announced on Form 8-K the purchase of Super Insight Limited pursuant to which we purchased a portion of a newly-constructed commercial building in exchange for our 80% interest in Lenton Fibre Optics Development Limited and $400,000 paid by us in cash. Lenton's primary asset is an undeveloped industrially zoned land parcel. Concurrently with the consummation of the transaction, Immtech Hong Kong Limited, Lenton's wholly-owned subsidiary, was transferred to us and is now directly held. On December 3, 2003, we announced on Form 8-K, the consummation of a Testing Agreement with Medicines For Malaria Venture and The University of North Carolina at Chapel Hill pursuant to which we, with the support of MMV and UNC, will conduct a proof of concept study of the dicationic drug candidate DB289 for the treatment of malaria. On January 21, 2004, we announced on Form 8-K the offering of a $5 million private placement of our Series D Convertible Preferred Stock and related warrants. On January 22, 2004 the offering was completed and closed. -77- SIGNATURES Pursuant to the requirements of Section 13 or 15(d) of the Securities Exchange Act of 1934, the registrant has duly caused this report to be signed on its behalf by the undersigned, thereunto duly authorized. IMMTECH INTERNATIONAL, INC. Date: June 14, 2004 By: /s/ T. Stephen Thompson ---------------------------------- ---------------------------------- T. Stephen Thompson Chief Executive Officer and President Pursuant to the requirements of the Securities Exchange Act of 1934, this report has been signed below by the following persons on behalf of the registrant and in the capacities and on the dates indicated. Signature Date --------- ---- /s/ T. Stephen Thompson June 14, 2004 ------------------------------------------------ -------------------------- T. Stephen Thompson Chief Executive Officer and President (Principal Executive Officer) /s/ Gary C. Parks June 14, 2004 ------------------------------------------------ -------------------------- Gary C. Parks Treasurer, Secretary and Chief Financial Officer (Principal Financial and Accounting Officer) /s/ Cecilia Chan June 14, 2004 ------------------------------------------------ -------------------------- Cecilia Chan Director /s/ Harvey Colten, MD June 14, 2004 ------------------------------------------------ -------------------------- Harvey Colten, MD Director /s/ Judy Lau June 14, 2004 ------------------------------------------------ -------------------------- Judy Lau Director /s/ Levi H.K. Lee, MD June 14, 2004 ------------------------------------------------ -------------------------- Levi H.K. Lee, MD Director /s/ Eric L. Sorkin June 14, 2004 ------------------------------------------------ -------------------------- Eric L. Sorkin Director /s/ Frederick W. Wackerle June 14, 2004 ------------------------------------------------ -------------------------- Frederick W. Wackerle Director EXHIBIT INDEX EXHIBIT NUMBER DESCRIPTION OF EXHIBIT -------------- ---------------------- 3.1 (2) Certificate of Incorporation of the Company, as amended 3.2 (8) By-laws of the Company, with amendment 3.3 (18) Amended and Restated Certificate of Incorporation of the Company, dated June 14, 2004 4.1 (3) Form of Common Stock Certificate 4.2 (2) Warrant Agreement relating to the Underwriters' Warrants 4.3 (2) Warrant Agreement, dated July 24, 1998, by and between the Company and RADE Management Corporation 4.4 (2) Warrant Agreement, dated October 12, 1998, by and between the Company and RADE Management Corporation 4.5 (8) Warrant Agreement, dated March 15, 2001, by and between the Company and The Kriegsman Group 4.6 (8) Warrant Agreement, dated July 31, 2000, by and between the Company and Griffith Shelmire Partners, Inc. 4.7 (8) Warrant Agreement, dated July 31, 2000, by and between the Company and Scott R. Griffith 4.8 (8) Warrant Agreement, dated July 31, 2000, by and between the Company and Jesse B. Shelmire 4.9 (9) Certificate of Designation for Series A Convertible Preferred Stock Private Placement, dated February 14, 2002 4.10 (9) Stock Purchase Warrant, dated February 14, 2002, for Series A Convertible Preferred Stock Private Placement 4.11 (11) Certificate of Designation for Series B Convertible Preferred Stock Private Placement, dated September 25, 2002 4.12 (11) Stock Purchase Warrant, dated September 25, 2002, for Series B Convertible Preferred Stock Private Placement 4.13 (12) Certificate of Designation for Series C Convertible Preferred Stock Private Placement, dated June 6, 2003 4.14 (17) Certificate of Designation for Series D Convertible Preferred Stock Private Placement, dated January 15, 2004 4.15 (17) Stock Purchase Warrant, dated January 15, 2004, for Series D Convertible Preferred Stock Private Placement 10.1 (1) Letter Agreement, dated January 15, 1997, by and between the Company, Pharm-Eco Laboratories, Inc. and The University of North Carolina at Chapel Hill, as amended 10.1 (1) Consulting Agreement, dated May 15, 1998, by and between the Company and RADE Management Corporation 10.2 (1) 1993 Stock Option and Award Plan 10.3 (6) 2000 Stock Option and Award Plan 10.4 (1) Letter Agreement, dated May 29, 1998, between the Company and Franklin Research Group, Inc. 10.5 (1) Indemnification Agreement, dated June 1, 1998, between the Company and RADE Management Corporation 10.6 (1) Letter Agreement, dated June 24, 1998, between the Company and Criticare Systems, Inc. 10.7 (1) Letter Agreement, dated June 25, 1998, between the Company and Criticare Systems, Inc. 10.8 (2) Amendment, dated January 15, 1999, to Letter Agreement between the Company, Pharm-Eco Laboratories, Inc. and The University of North Carolina at Chapel Hill, as amended 10.9 (5) Office Lease, dated August 26, 1999, by and between the Company and Arthur J. Rogers & Co. 10.10 (8) License Agreement, dated August 25, 1993, by and between the University of North Carolina at Chapel Hill and Pharm-Eco Laboratories, Inc. 10.11 (8) Assignment Agreement, dated as of March 27, 2001, by and between the Company and Pharm-Eco Laboratories, Inc. 10.12 (8) Clinical Research Subcontract, dated as of March 29, 2001, by and between The University of North Carolina at Chapel Hill and the Company 10.13 (1) Material Transfer and Option Agreement, dated March 23, 1998, by and between the Company and Sigma Diagnostics, Inc. 10.14 (1) License Agreement, dated March 10, 1998, by and between the Company and Northwestern University 10.15 (1) License Agreement, dated October 27, 1994, by and between the Company and Northwestern University 10.16 (1) Assignment of Intellectual Properties, dated June 29, 1998, between the Company and Criticare Systems, Inc. 10.18 (1) Assignment Agreement, dated June 26, 1998, by and between the Company and Criticare Systems, Inc. 10.19 (1) Assignment Agreement, dated June 29, 1998, by and between the Company and Criticare Systems, Inc. 10.20 (1) International Patent, Know-How and Technology License Agreement, dated June 29, 1998, by and between the Company and Criticare Systems, Inc. 10.21 (1) Employment Agreement, dated 1992, by and between the Company and T. Stephen Thompson 10.22 (2) Funding and Research Agreement, dated September 30, 1998, by and among the Company, NextEra Therapeutics, Inc. and Franklin Research Group, Inc. 10.23 (4) Two Year Plus 200% Lock-Up Agreement executed by James Ng 10.24 (4) Employment Agreement, dated 1998, by and between NextEra and Lawrence Potempa 10.25 (7) Form of Regulation D Subscription Agreement for December 8, 2000 Private Placement 10.26 (7) Form of Regulation S Subscription Agreement for December 8, 2000 Private Placement 10.27 (9) Form of Regulation D Subscription Agreement for February 14, 2002 Series A Preferred Private Placement 10.28 (9) Form of Regulation S Subscription Agreement for February 14, 2002 Series A Preferred Private Placement 10.29 (10) Amendment, dated January 28, 2002, to License Agreement between the Company, Pharm-Eco Laboratories, Inc. and The University of North Carolina at Chapel Hill, as amended 10.30 (11) Form of Regulation D Subscription Agreement for September 2002 Series B Preferred Private Placement 10.31 (11) Form of Regulation S Subscription Agreement for September 2002 Series B Preferred Private Placement 10.32 (12) Form of Regulation D Subscription Agreement for June 2003 Series C Preferred Private Placement 10.33 (12) Form of Regulation S Subscription Agreement for June 2003 Series C Preferred Private Placement 10.34 (14) Regis Pharmaceutical Manufacturing Agreement dated March 4, 2003 10.35 (15) Share Purchase Agreement and Deed of Indemnity as related to shares in Super Insight Limited, dated November 28, 2003, by and between the Company, Chan Kon Fung and Super Insight Limited 10.36 (15) Allonge to the Share Purchase Agreement and Deed of Indemnity as related to shares in Super Insight Limited and Immtech Hong Kong Limited, dated November 28, 2003, by and between the Company, Chan Kon Fung, Lenton Fibre Optics Development Limited, Super Insight Limited, and Immtech Hong Kong Limited 10.37 (16) Testing Agreement, dated as of November 26, 2003, by and between Medicines for Malaria Venture, Immtech International Inc., and The University of North Carolina at Chapel Hill 10.38 (17) Form of Regulation D Subscription Agreement for January 2004 Series D Preferred Private Placement 10.39 (17) Form of Regulation S Subscription Agreement for January 2004 Series D Preferred Private Placement 14.1 (18) Code of Ethics 21.1 (13) Subsidiaries of Registrant 23.1 (18) Consent of Deloitte & Touche LLP 31.1 (18) Certification of Chief Executive Officer pursuant to Section 302 of the Sarbanes-Oxley Act of 2002 31.2 (18) Certification of Chief Financial Officer pursuant to Section 302 of the Sarbanes-Oxley Act of 2002 32.1 (18) Certification of Chief Executive Officer pursuant to Section 906 of the Sarbanes-Oxley Act of 2002 32.2 (18) Certification of Chief Financial Officer pursuant to Section 906 of the Sarbanes-Oxley Act of 2002 (1) Incorporated by Reference to our Registration Statement on Form SB-2 (Registration Statement No. 333-64393), as filed with the Securities and Exchange Commission on September 28, 1998. (2) Incorporated by Reference to Amendment No. 1 to our Registration Statement on Form SB-2 (Registration Statement No. 333-64393), as filed with the Securities and Exchange Commission on February 11, 1999. (3) Incorporated by Reference to Amendment No. 2 our Registration Statement on Form SB-2 (Registration Statement No. 333-64393), as filed with the Securities and Exchange Commission on March 30, 1999. (4) Incorporated by Reference to our Form 10-KSB for the fiscal year ended March 31, 1999 (File No. 001-14907), as filed with the Securities and Exchange Commission on June 29, 1999. (5) Incorporated by Reference to our Annual Report on Form 10-KSB for the fiscal year ended March 31, 2000 (File No. 000-25669), as filed with the Securities and Exchange Commission on June 26, 2000. (6) Incorporated by Reference to Annex A to our Definitive Proxy Statement (File No. 000-25669), as filed with the Securities and Exchange Commission on August 25, 2000. (7) Incorporated by Reference to our Quarterly Report on Form 10-QSB (File No. 000-25669), as filed with the Securities and Exchange Commission on February 14, 2001. (8) Incorporated by Reference to our Annual Report on Form 10-KSB/A (File No. 000-25669), as filed with the Securities and Exchange Commission on June 29, 2001, as amended on July 6, 2001. (9) Incorporated by Reference to our Form 8-K (File No. 000-25669), as filed with the Securities and Exchange Commission on February 14, 2002. (10) Incorporated by Reference to our Form 10-Q (File No. 000-25669), as filed with the Securities and Exchange Commission on February 14, 2002, as amended on June 10, 2002. (11) Incorporated by Reference to our Form 8-K (File No. 001-14907), as filed with the Securities and Exchange Commission on September 25, 2002. (12) Incorporated by Reference to our Form 8-K (File No. 001-14907), as filed with the Securities and Exchange Commission on June 10, 2003. (13) Incorporated by Reference to our Form 10-K (File No. 001-14907), as filed with the Securities and Exchange Commission on June 27, 2003, as amended on October 15, 2003. (14) Incorporated by Reference to our Form 10-K/A (File No. 001-14907), as filed with the Securities and Exchange Commission on October 15, 2003. (15) Incorporated by Reference to our Form 8-K (File No. 001-14907), as filed with the Securities and Exchange Commission on December 2, 2003. (16) Incorporated by Reference to our Form 8-K (File No. 001-14907), as filed with the Securities and Exchange Commission on December 3, 2003. (17) Incorporated by Reference to our Form 8-K (File No. 001-14907), as filed with the Securities and Exchange Commission on January 21, 2004. (18) Filed herewith. IMMTECH INTERNATIONAL, INC. AND SUBSIDIARIES (A Development Stage Enterprise) Consolidated Financial Statements as of March 31, 2003 and 2004, for the Years Ended March 31, 2002, 2003 and 2004 and for the Period October 15, 1984 (Date of Inception) to March 31, 2004 (Unaudited) and Report of Independent Registered Public Accounting Firm IMMTECH INTERNATIONAL, INC. AND SUBSIDIARIES (A Development Stage Enterprise) TABLE OF CONTENTS -------------------------------------------------------------------------------- Page REPORT OF INDEPENDENT REGISTERED PUBLIC ACCOUNTING FIRM 1 CONSOLIDATED FINANCIAL STATEMENTS AS OF MARCH 31, 2003 AND 2004, FOR THE YEARS ENDED MARCH 31, 2002, 2003 AND 2004, AND FOR THE PERIOD FROM OCTOBER 15, 1984 (DATE OF INCEPTION) TO MARCH 31, 2004 (UNAUDITED): Balance Sheets 2 Statements of Operations 3 Statements of Stockholders' Equity (Deficiency in Assets) 4-7 Statements of Cash Flows 8 Notes to Financial Statements 9-35 REPORT OF INDEPENDENT REGISTERED PUBLIC ACCOUNTING FIRM To the Board of Directors of Immtech International, Inc.: We have audited the accompanying consolidated balance sheets of Immtech International, Inc. (a development stage enterprise) and subsidiaries (the "Company") as of March 31, 2003 and 2004, and the related consolidated statements of operations, stockholders' equity (deficiency in assets) and cash flows for each of the three years in the period ended March 31, 2004. These financial statements are the responsibility of the Company's management. Our responsibility is to express an opinion on these financial statements based on our audits. We conducted our audits in accordance with standards of the Public Company Accounting Oversight Board (United States). Those standards require that we plan and perform the audit to obtain reasonable assurance about whether the financial statements are free of material misstatement. An audit includes examining, on a test basis, evidence supporting the amounts and disclosures in the financial statements. An audit also includes assessing the accounting principles used and significant estimates made by management, as well as evaluating the overall financial statement presentation. We believe that our audits provide a reasonable basis for our opinion. In our opinion, such consolidated financial statements present fairly, in all material respects, the financial position of the Company as of March 31, 2003 and 2004, and the results of its operations and its cash flows for each of the three years in the period ended March 31, 2004, in conformity with accounting principles generally accepted in the United States of America. Milwaukee, Wisconsin June 4, 2004 IMMTECH INTERNATIONAL, INC. AND SUBSIDIARIES (A Development Stage Enterprise) CONSOLIDATED BALANCE SHEETS MARCH 31, 2003 AND 2004 -------------------------------------------------------------------------------- ASSETS 2003 2004 ----------- ----------- CURRENT ASSETS: Cash and cash equivalents $ 112,040 $ 6,745,283 Restricted funds on deposit 2,739,947 2,154,928 Other current assets 133,525 59,979 ----------- ----------- Total current assets 2,985,512 8,960,190 PROPERTY AND EQUIPMENT - Net 3,604,656 3,610,214 OTHER ASSETS 19,848 15,477 ----------- ----------- TOTAL ASSETS $ 6,610,016 $12,585,881 =========== =========== See notes to consolidated financial statements. -------------------------------------------------------------------------------- LIABILITIES AND STOCKHOLDERS' EQUITY 2003 2004 ------------ ------------ CURRENT LIABILITIES: Accounts payable $ 541,881 $ 970,308 Accrued expenses 4,821 22,382 Deferred revenue 2,554,071 1,831,093 ------------ ------------ Total current liabilities 3,100,773 2,823,783 DEFERRED RENTAL OBLIGATION 20,779 14,413 ------------ ------------ Total liabilities 3,121,552 2,838,196 ------------ ------------ COMMITMENTS AND CONTINGENCIES MINORITY INTEREST 296,193 STOCKHOLDERS' EQUITY: Preferred stock, par value $0.01 per share, 4,440,000 and 4,080,000 shares authorized and unissued as of March 31, 2003 and 2004, respectively Series A convertible preferred stock, par value $0.01 per share, stated value $25 per share, 320,000 shares authorized, 142,800 and 80,800 shares issued and outstanding as of March 31, 2003 and 2004, respectively, aggregate liquidation preference of $3,668,005 and $2,075,250 as of March 31, 2003 and 2004, respectively 3,668,005 2,075,250 Series B convertible preferred stock, par value $0.01 per share, stated value $25 per share, 240,000 shares authorized, 56,725 and 19,925 shares issued and outstanding as of March 31, 2003 and 2004, respectively, aggregated liquidation preference of $1,469,967 and $516,093 as of March 31, 2003 and 2004, respectively 1,469,967 516,093 Series C convertible preferred stock, par value $0.01 per share, stated value $25 per share, 160,000 shares authorized, 72,304 shares outstanding as of March 31, 2004, aggregate liquidation preference of $1,874,186 as of March 31, 2004 1,874,186 Series D convertible preferred stock, par value $0.01 per share, stated value $25 per share, 200,000 shares authorized, 200,000 shares outstanding as of March 31, 2004, aggregate liquidation preference of $5,056,712 as of March 31, 2004 5,056,712 Common stock, par value $0.01 per share, 100,000,000 shares authorized, 7,898,986 and 9,835,286 shares issued and outstanding as of March 31, 2003 and 2004, respectively 78,990 98,353 Additional paid-in capital 40,142,617 58,666,489 Deficit accumulated during the developmental stage (42,167,308) (58,539,398) ------------ ------------ Total stockholders' equity 3,192,271 9,747,685 ------------ ------------ TOTAL LIABILITIES AND STOCKHOLDERS' EQUITY $ 6,610,016 $ 12,585,881 ============ ============ -2- IMMTECH INTERNATIONAL, INC. AND SUBSIDIARIES (A Development Stage Enterprise) CONSOLIDATED STATEMENTS OF OPERATIONS YEARS ENDED MARCH 31, 2002, 2003 AND 2004 AND THE PERIOD OCTOBER 15, 1984 (DATE OF INCEPTION) TO MARCH 31, 2004 (UNAUDITED) -------------------------------------------------------------------------------- October 15, 1984 (Inception) Years Ended March 31, to March 31, -------------------------------------------- 2002 2003 2004 2004 ------------ ------------ ------------ ------------ REVENUES $ 3,522,113 $ 1,608,849 $ 2,416,180 $ 11,259,002 EXPENSES: Research and development 3,958,107 2,570,370 3,292,737 34,364,268 General and administrative 2,927,726 3,731,398 11,989,670 33,061,554 Equity in loss of joint venture 135,002 ------------ ------------ ------------ ------------ Total expenses 6,885,833 6,301,768 15,282,407 67,560,824 ------------ ------------ ------------ ------------ LOSS FROM OPERATIONS (3,363,720) (4,692,919) (12,866,227) (56,301,822) OTHER INCOME (EXPENSE): Interest income 40,610 13,850 20,414 597,992 Interest expense (1,129,502) Loss on sales of investment securities - net (2,942) Cancelled offering costs (584,707) Gain on extinguishment of debt 1,427,765 ------------ ------------ ------------ ------------ Other income (expense) - net 40,610 13,850 20,414 308,606 ------------ ------------ ------------ ------------ NET LOSS (3,323,110) (4,679,069) (12,845,813) (55,993,216) CONVERTIBLE PREFERRED STOCK DIVIDENDS AND CONVERTIBLE PREFERRED STOCK PREMIUM DEEMED DIVIDENDS (937,935) (451,869) (3,526,277) (4,916,081) REDEEMABLE PREFERRED STOCK CONVERSION, PREMIUM AMORTIZATION AND DIVIDENDS 2,369,899 NET LOSS ATTRIBUTABLE TO COMMON STOCKHOLDERS $ (4,261,045) $ (5,130,938) $(16,372,090) $(58,539,398) ============ ------------ ------------ ------------ BASIC AND DILUTED NET LOSS PER SHARE ATTRIBUTABLE TO COMMON STOCKHOLDERS: Net loss $ (0.55) $ (0.71) $ (1.43) Convertible preferred stock dividends and convertible preferred stock premium deemed dividends (0.16) (0.07) (0.39) ------------ ------------ ------------ BASIC AND DILUTED NET LOSS PER SHARE ATTRIBUTABLE TO COMMON STOCKHOLDERS $ (0.71) $ (0.78) $ (1.82) ============ ------------ ------------ WEIGHTED AVERAGE SHARES USED IN COMPUTING BASIC AND DILUTED NET LOSS PER SHARE 6,011,416 6,565,495 8,977,817 See notes to consolidated financial statements. -3- IMMTECH INTERNATIONAL, INC. AND SUBSIDIARIES (A Development Stage Enterprise) CONSOLIDATED STATEMENTS OF STOCKHOLDERS' EQUITY (DEFICIENCY IN ASSETS) YEARS ENDED MARCH 31, 2002, 2003 AND 2004 AND THE PERIOD OCTOBER 15, 1984 (DATE OF INCEPTION) TO MARCH 31, 2004 (UNAUDITED) ----------------------------------------------------------------------------------------------------------------------------------- Series A Convertible Series B Convertible Series C Convertible Preferred Stock Preferred Stock Preferred Stock -------------------------- -------------------------- -------------------------- Issued and Issued and Issued and Outstanding Amount Outstanding Amount Outstanding Amount October 15, 1984 (Inception) Issuance of common stock to founders Balance, March 31, 1985 Issuance of common stock Net loss Balance, March 31, 1986 Issuance of common stock Net loss Balance, March 31, 1987 Issuance of common stock Net loss Balance, March 31, 1988 Issuance of common stock Provision for compensation Net loss Balance, March 31, 1989 Issuance of common stock Provision for compensation Net loss Balance, March 31, 1990 Issuance of common stock Provision for compensation Net loss Balance, March 31, 1991 Issuance of common stock Provision for compensation Issuance of stock options in exchange for cancellation of indebtedness Net loss Balance, March 31, 1992 Issuance of common stock Provision for compensation Net loss Balance, March 31, 1993 Issuance of common stock Provision for compensation Net loss Balance, March 31, 1994 Net loss Balance, March 31, 1995 Issuance of common stock for compensation Net loss Balance, March 31, 1996 Issuance of common stock Provision for compensation - employees Provision for compensation - nonemployees Issuance of warrants to purchase common stock Net loss Balance, March 31, 1997 Exercise of options Provision for compensation - employees Provision for compensation - nonemployees Contributed capital - common stockholders Net loss Balance, March 31, 1998 Issuance of common stock under private placement offering Exercise of options Provision for compensation - nonemployees Issuance of common stock to Criticare Conversion of Criticare debt to common stock Conversion of debt to common stock Conversion of redeemable preferred stock to common stock Net loss Balance, March 31, 1999 Comprehensive loss: Net loss Other comprehensive loss: Unrealized loss on investment securities available for sale Comprehensive loss Issuance of common stock under initial public offering, less offering costs of $513,000 Exercise of options and warrants Provision for compensation - nonemployees Issuance of common stock for compensation - nonemployees Issuance of common stock for accrued interest Balance, March 31, 2000 Comprehensive loss: Net loss Other comprehensive income (loss): Unrealized loss on investment securities available for sale Reclassification adjustment for loss included in net loss Comprehensive loss Issuance of common stock under private placement offering Exercise of options Provision for compensation - nonemployees Contributed capital - common stockholder Balance, March 31, 2001 Net loss Issuance of Series A convertible preferred stock under private placement offerings, less cash offering costs of $153,985 160,100 $ 4,002,500 Issuance of common stock as offering costs under private placement offerings Accrual of preferred stock dividends 29,400 Exercise of options Provision for compensation - nonemployees ----------- ----------- Balance, March 31, 2002 160,100 $ 4,031,900 Net loss Issuance of Series B convertible preferred stock under private placement offerings, less cash offering costs of $58,792 76,725 $ 1,918,125 Issuance of common stock for services provided in connection with private placement offerings Conversion of convertible preferred stock to common stock (17,300) (437,396) (20,000) (515,671) Accrual of preferred stock dividends 226,210 76,227 Payment of preferred stock dividends (152,709) (8,714) Issuance of common stock for land use rights acquisition Issuance of common stock and warrants for services Exercise of options Provision for compensation - nonemployees ----------- ----------- ----------- ----------- Balance, March 31, 2003 142,800 3,668,005 56,725 1,469,967 Net loss Issuance of Series C convertible preferred stock under private placement offerings, less offering costs of $1,685,365 (including cash of $289,000) 125,352 $ 3,133,800 Issuance of Series D convertible preferred stock under private placement offerings, less cash offering costs of $428,919 Issuance of common stock for services provided in connection with private placement offerings Conversion of convertible preferred stock to common stock (62,000) (1,566,440) (36,800) (939,231) (53,048) (1,344,792) Accrual of preferred stock dividends 147,311 53,533 175,157 Payment of preferred stock dividends (173,626) (68,176) (89,979) Exercise of warrants Issuance of common stock and warrants for services - nonemployees Exercise of options Provision for compensation - nonemployees ----------- ----------- ----------- ----------- ----------- ----------- Balance, March 31, 2004 80,800 $ 2,075,250 19,925 $ 516,093 72,304 $ 1,874,186 =========== =========== =========== =========== =========== =========== ------------------------------------------------------------------- Series D Convertible Preferred Stock Common Stock --------------------------- -------------------- Additional Issued and Issued and Paid-in Outstanding Amount Outstanding Amount Capital October 15, 1984 (Inception) Issuance of common stock to founders 113,243 $ 1,132 $ 24,868 --------- ------- ------------ Balance, March 31, 1985 113,243 1,132 24,868 Issuance of common stock 85,368 854 269,486 Net loss --------- ------- ------------ Balance, March 31, 1986 198,611 1,986 294,354 Issuance of common stock 42,901 429 285,987 Net loss --------- ------- ------------ Balance, March 31, 1987 241,512 2,415 580,341 Issuance of common stock 4,210 42 28,959 Net loss --------- ------- ------------ Balance, March 31, 1988 245,722 2,457 609,300 Issuance of common stock 62,792 628 569,372 Provision for compensation 489,975 Net loss --------- ------- ------------ Balance, March 31, 1989 308,514 3,085 1,668,647 Issuance of common stock 16,478 165 171,059 Provision for compensation 320,980 Net loss --------- ------- ------------ Balance, March 31, 1990 324,992 3,250 2,160,686 Issuance of common stock 218 2 1,183 Provision for compensation 6,400 Net loss --------- ------- ------------ Balance, March 31, 1991 325,210 3,252 2,168,269 Issuance of common stock 18,119 181 85,774 Provision for compensation 864,496 Issuance of stock options in exchange for cancellation of indebtedness 57,917 Net loss --------- ------- ------------ Balance, March 31, 1992 343,329 3,433 3,176,456 Issuance of common stock 195,790 1,958 66,839 Provision for compensation 191,502 Net loss --------- ------- ------------ Balance, March 31, 1993 539,119 5,391 3,434,797 Issuance of common stock 107,262 1,073 40,602 Provision for compensation 43,505 Net loss --------- ------- ------------ Balance, March 31, 1994 646,381 $ 6,464 $ 3,518,904 Net loss --------- ------- ------------ Balance, March 31, 1995 646,381 6,464 3,518,904 Issuance of common stock for compensation 16,131 161 7,339 Net loss --------- ------- ------------ Balance, March 31, 1996 662,512 6,625 3,526,243 Issuance of common stock 12,986 130 5,908 Provision for compensation - employees 45,086 Provision for compensation - nonemployees 62,343 Issuance of warrants to purchase common stock 80,834 Net loss --------- ------- ------------ Balance, March 31, 1997 675,498 6,755 3,720,414 Exercise of options 68,167 682 28,862 Provision for compensation - employees 50,680 Provision for compensation - nonemployees 201,696 Contributed capital - common stockholders 231,734 Net loss --------- ------- ------------ Balance, March 31, 1998 743,665 7,437 4,233,386 Issuance of common stock under private placement offering 575,000 5,750 824,907 Exercise of options 40,650 406 12,944 Provision for compensation - nonemployees 2,426,000 Issuance of common stock to Criticare 86,207 862 133,621 Conversion of Criticare debt to common stock 180,756 1,808 856,485 Conversion of debt to common stock 424,222 4,242 657,555 Conversion of redeemable preferred stock to common stock 1,195,017 11,950 1,852,300 Net loss --------- ------- ------------ Balance, March 31, 1999 3,245,517 $32,455 $ 10,997,198 Comprehensive loss: Net loss Other comprehensive loss: Unrealized loss on investment securities available for sale Comprehensive loss Issuance of common stock under initial public offering, less offering costs of $513,000 1,150,000 11,500 9,161,110 Exercise of options and warrants 247,420 2,474 424,348 Provision for compensation - nonemployees 509,838 Issuance of common stock for compensation - nonemployees 611,250 6,113 6,106,387 Issuance of common stock for accrued interest 28,147 281 281,189 --------- ------- ------------ Balance, March 31, 2000 5,282,334 52,823 27,480,070 Comprehensive loss: Net loss Other comprehensive income (loss): Unrealized loss on investment securities available for sale Reclassification adjustment for loss included in net loss Comprehensive loss Issuance of common stock under private placement offering 584,250 5,843 4,299,806 Exercise of options 88,661 886 41,922 Provision for compensation - nonemployees 1,739,294 Contributed capital - common stockholder 13,825 --------- ------- ------------ Balance, March 31, 2001 5,955,245 59,552 33,574,917 Net loss Issuance of Series A convertible preferred stock under private placement offerings, less cash offering costs of $153,985 754,550 Issuance of common stock as offering costs under private placement offerings 60,000 600 (600) Accrual of preferred stock dividends Exercise of options 51,214 512 18,972 Provision for compensation - nonemployees 332,005 --------- ------- ------------ Balance, March 31, 2002 6,066,459 $60,664 $ 34,679,844 Net loss Issuance of Series B convertible preferred stock under private placement offerings, less cash offering costs of $58,792 90,640 Issuance of common stock for services provided in connection with private placement offerings 290,000 2,900 942,200 Conversion of convertible preferred stock to common stock 228,448 2,285 950,758 Accrual of preferred stock dividends Payment of preferred stock dividends 45,529 456 160,657 Issuance of common stock for land use rights acquisition 1,260,000 12,600 2,986,200 Issuance of common stock and warrants for services 8,333 83 89,042 Exercise of options 217 2 126 Provision for compensation - nonemployees 243,150 --------- ------- ------------ Balance, March 31, 2003 7,898,986 78,990 40,142,617 Net loss Issuance of Series C convertible preferred stock under private placement offerings, less offering costs of $1,685,365 (including cash of $289,000) (565,088) Issuance of Series D convertible preferred stock under private placement offerings, less cash offering costs of $428,919 200,000 $ 5,000,000 1,544,368 Issuance of common stock for services provided in connection with private placement offerings 220,000 2,200 1,394,800 Conversion of convertible preferred stock to common stock 887,817 8,878 3,841,327 Accrual of preferred stock dividends 56,712 Payment of preferred stock dividends 44,398 443 330,197 Exercise of warrants 559,350 5,594 4,468,572 Issuance of common stock and warrants for services - nonemployees 201,667 2,017 7,231,835 Exercise of options 23,068 231 10,361 Provision for compensation - nonemployees 267,500 ------------ ------------ --------- ------- ------------ Balance, March 31, 2004 200,000 $ 5,056,712 9,835,286 $98,353 $ 58,666,489 ============ ============ ========= ======= ============ Deficit Accumulated Total Accumulated Other Stockholders' During the Comprehensive Equity Development Income (Deficiency in Stage (Loss) Assets) October 15, 1984 (Inception) Issuance of common stock to founders $ 26,000 ------------ Balance, March 31, 1985 26,000 Issuance of common stock 270,340 Net loss $ (209,569) (209,569) ------------ ------------ Balance, March 31, 1986 (209,569) 86,771 Issuance of common stock 286,416 Net loss (47,486) (47,486) ------------ ------------ Balance, March 31, 1987 (257,055) 325,701 Issuance of common stock 29,001 Net loss (294,416) (294,416) ------------ ------------ Balance, March 31, 1988 (551,471) 60,286 Issuance of common stock 570,000 Provision for compensation 489,975 Net loss (986,746) (986,746) ------------ ------------ Balance, March 31, 1989 (1,538,217) 133,515 Issuance of common stock 171,224 Provision for compensation 320,980 Net loss (850,935) (850,935) ------------ ------------ Balance, March 31, 1990 (2,389,152) (225,216) Issuance of common stock 1,185 Provision for compensation 6,400 Net loss (163,693) (163,693) ------------ ------------ Balance, March 31, 1991 (2,552,845) (381,324) Issuance of common stock 85,955 Provision for compensation 864,496 Issuance of stock options in exchange for cancellation of indebtedness 57,917 Net loss (1,479,782) (1,479,782) ------------ ------------ Balance, March 31, 1992 (4,032,627) (852,738) Issuance of common stock 68,797 Provision for compensation 191,502 Net loss (1,220,079) (1,220,079) ------------ ------------ Balance, March 31, 1993 (5,252,706) (1,812,518) Issuance of common stock 41,675 Provision for compensation 43,505 Net loss (2,246,426) (2,246,426) ------------ ------------ (Continued) Balance, March 31, 1994 $ (7,499,132) $ (3,973,764) Net loss (1,661,677) (1,661,677) ------------ ------------ Balance, March 31, 1995 (9,160,809) (5,635,441) Issuance of common stock for compensation 7,500 Net loss (1,005,962) (1,005,962) ------------ ------------ Balance, March 31, 1996 (10,166,771) (6,633,903) Issuance of common stock 6,038 Provision for compensation - employees 45,086 Provision for compensation - nonemployees 62,343 Issuance of warrants to purchase common stock 80,834 Net loss (1,618,543) (1,618,543) ------------ ------------ Balance, March 31, 1997 (11,785,314) (8,058,145) Exercise of options 29,544 Provision for compensation - employees 50,680 Provision for compensation - nonemployees 201,696 Contributed capital - common stockholders 231,734 Net loss (1,477,132) (1,477,132) ------------ ------------ Balance, March 31, 1998 (13,262,446) (9,021,623) Issuance of common stock under private placement offering 830,657 Exercise of options 13,350 Provision for compensation - nonemployees 2,426,000 Issuance of common stock to Criticare 134,483 Conversion of Criticare debt to common stock 858,293 Conversion of debt to common stock 661,797 Conversion of redeemable preferred stock to common stock 3,713,334 5,577,584 Net loss (1,929,003) (1,929,003) ------------ ------------ (Continued) Balance, March 31, 1999 (11,478,115) $ (448,462) Comprehensive loss: -- Net loss (11,433,926) (11,433,926) Other comprehensive loss: Unrealized loss on investment securities available for sale $ (1,178) (1,178) ------------ Comprehensive loss (11,435,104) Issuance of common stock under initial public offering, less offering costs of $513,000 9,172,610 Exercise of options and warrants 426,822 Provision for compensation - nonemployees 509,838 Issuance of common stock for compensation - nonemployees 6,112,500 Issuance of common stock for accrued interest 281,470 ------------ -------------- ------------ Balance, March 31, 2000 (22,912,041) (1,178) 4,619,674 ------------ Comprehensive loss: Net loss (9,863,284) (9,863,284) Other comprehensive income (loss): Unrealized loss on investment securities available for sale (1,764) (1,764) Reclassification adjustment for loss included in net loss 2,942 2,942 -------------- ------------ Comprehensive loss (9,862,106) Issuance of common stock under private placement offering 4,305,649 Exercise of options 42,808 Provision for compensation - nonemployees 1,739,294 Contributed capital - common stockholder 13,825 ------------ -------------- ------------ Balance, March 31, 2001 (32,775,325) 859,144 Net loss (3,323,110) (3,323,110) Issuance of Series A convertible preferred stock under private placement offerings, less cash offering costs of $153,985 (908,535) 3,848,515 Issuance of common stock as offering costs under private placement offerings Accrual of preferred stock dividends (29,400) Exercise of options 19,484 Provision for compensation - nonemployees 332,005 ------------ -------------- ------------ (Continued) Balance, March 31, 2002 $(37,036,370) $ 1,736,038 Net loss (4,679,069) (4,679,069) Issuance of Series B convertible preferred stock under private placement offerings, less cash offering costs of $58,792 (149,432) 1,859,333 Issuance of common stock for services provided in connection with private placement offerings 945,100 Conversion of convertible preferred stock to common stock (24) Accrual of preferred stock dividends (302,437) Payment of preferred stock dividends (310) Issuance of common stock for land use rights acquisition 2,998,800 Issuance of common stock and warrants for services 89,125 Exercise of options 128 Provision for compensation - nonemployees 243,150 ------------ -------------- ------------ Balance, March 31, 2003 (42,167,308) 3,192,271 Net loss (12,845,813) (12,845,813) Issuance of Series C convertible preferred stock under private placement offerings, less offering costs of $1,685,365 (including cash of $289,000) (1,120,277) 1,448,435 Issuance of Series D convertible preferred stock under private placement offerings, less cash offering costs of $428,919 (1,973,287) 4,571,081 Issuance of common stock for services provided in connection with private placement offerings 1,397,000 Conversion of convertible preferred stock to common stock (258) Accrual of preferred stock dividends (432,713) Payment of preferred stock dividends (1,141) Exercise of warrants 4,474,166 Issuance of common stock and warrants for services - nonemployees 7,233,852 Exercise of options 10,592 Provision for compensation - nonemployees 267,500 ------------ -------------- ------------ Balance, March 31, 2004 $(58,539,398) $ 0 $ 9,747,685 ============ ============== ============ (Concluded) See notes to consolidated financial statements. -4- IMMTECH INTERNATIONAL, INC. AND SUBSIDIARIES (A Development Stage Enterprise) CONSOLIDATED STATEMENTS OF CASH FLOWS YEARS ENDED MARCH 31, 2002, 2003 AND 2004 AND THE PERIOD OCTOBER 15, 1984 (DATE OF INCEPTION) TO MARCH 31, 2004 (UNAUDITED) October 15, 1984 (Inception) Years Ended March 31, to March 31, ---------------------------------------------- 2002 2003 2004 2004 ------------ ------------ ------------ ------------ OPERATING ACTIVITIES: Net loss $ (3,323,110) $ (4,679,069) $(12,845,813) $(55,993,216) Adjustments to reconcile net loss to net cash used in operating activities: Compensation recorded related to issuance of common stock, common stock options and warrants 332,005 1,277,375 7,501,352 22,361,327 Depreciation and amortization of property and equipment 98,893 93,420 115,261 752,441 Deferred rental obligation (6,366) (6,366) (6,366) 14,413 Equity in loss of joint venture 135,002 Loss on sales of investment securities - net 2,942 Amortization of debt discounts and issuance costs 134,503 Gain on extinguishment of debt (1,427,765) Changes in assets and liabilities: Restricted funds on deposit 3,210,153 (2,137,547) 585,019 (2,154,928) Other current assets (11,592) (93,644) 73,546 (59,979) Other assets 4,371 (15,477) Accounts payable (1,150,704) (4,741) 428,427 1,297,843 Accrued expenses (66,605) 564 17,561 685,395 Deferred revenue (2,945,759) 1,990,636 (722,978) 1,831,093 ------------ ------------ ------------ ------------ Net cash used in operating activities (3,863,085) (3,559,372) (4,849,620) (32,436,406) ------------ ------------ ------------ ------------ INVESTING ACTIVITIES: Purchase of property and equipment (64,819) (225,528) (417,012) (1,335,726) Advances to Joint Venture (135,002) Proceeds from maturities of investments 1,800,527 Purchases of investment securities (1,803,469) ------------ ------------ ------------ ------------ Net cash used in investing activities (64,819) (225,528) (417,012) (1,473,670) ------------ ------------ ------------ ------------ FINANCING ACTIVITIES: Net advances from stockholders and affiliates 985,172 Proceeds from issuance of notes payable 2,645,194 Principal payments on notes payable (218,119) Payments for debt issuance costs (53,669) Payments for extinguishment of debt (203,450) Net proceeds from issuance of redeemable preferred stock 3,330,000 Net proceeds from issuance of convertible preferred stock and warrants 3,848,515 1,859,333 7,416,516 13,124,364 Payments for convertible preferred stock dividends and for fractional shares of common stock resulting from the conversions of convertible preferred stock (334) (1,399) (1,733) Net proceeds from issuance of common stock 19,484 128 4,484,758 20,802,041 Additional capital contributed by stockholders 245,559 ------------ ------------ ------------ ------------ Net cash provided by financing activities 3,867,999 1,859,127 11,899,875 40,655,359 ------------ ------------ ------------ ------------ NET (DECREASE) INCREASE IN CASH AND CASH EQUIVALENTS (59,905) (1,925,773) 6,633,243 6,745,283 CASH AND CASH EQUIVALENTS, BEGINNING OF PERIOD 2,097,718 2,037,813 112,040 ------------ ------------ ------------ ------------ CASH AND CASH EQUIVALENTS, END OF PERIOD $ 2,037,813 $ 112,040 $ 6,745,283 $ 6,745,283 ============ ============ ============ ============ SUPPLEMENTAL CASH FLOW INFORMATION (Note 11) See notes to consolidated financial statements. -5- IMMTECH INTERNATIONAL, INC. AND SUBSIDIARIES (A Development Stage Enterprise) NOTES TO CONSOLIDATED FINANCIAL STATEMENTS YEARS ENDED MARCH 31, 2002, 2003 AND 2004 -------------------------------------------------------------------------------- 1. COMPANY BUSINESS AND SUMMARY OF SIGNIFICANT ACCOUNTING POLICIES Description of Business - Immtech International, Inc. (a development stage enterprise) and its subsidiaries (the "Company") is a pharmaceutical company advancing the development and commercialization of oral drugs to treat infectious diseases and metabolic (diabetes) and neoplastic (cancer) disorders. The Company has drug development programs that include treatments for fungal infections, malaria, tuberculosis, diabetes, Pneumocystis carinii pneumonia, and tropical medicine diseases including African sleeping sickness (a parasitic disease also known as Trypanosomiasis) and Leishmaniasis (a parasitic disease that can cause liver damage). The Company holds worldwide patents and patent applications, licenses and rights to license and technologies primarily from a scientific consortium that has granted it exclusive rights to commercialize products from, and license rights to, the technology. The Company is a development stage enterprise and since its inception on October 15, 1984, has engaged in research and development programs, expanding its network of scientists and scientific advisors, licensing technology agreements, and advancing the commercialization of its dication technology platform. The Company uses the expertise and resources of strategic partners and contracted parties in a number of areas, including: (i) laboratory research, (ii) pre-clinical and human clinical trials and (iii) manufacture of pharmaceutical drugs. The Company does not have any products currently available for sale, and no products are expected to be commercially available for sale until after March 31, 2005, if at all. Since inception, the Company has incurred accumulated losses of approximately $55,993,000. Management expects the Company to continue to incur significant losses during the next several years as the Company continues its commercialization, research and development activities and clinical trial efforts. In addition, the Company has various research and development agreements with third parties and is dependent on their ability to perform under these agreements. There can be no assurance that the Company's continued research will lead to the development of commercially viable products. The Company's operations to date have consumed substantial amounts of cash. The negative cash flow from operations is expected to continue in the foreseeable future. The Company will require substantial additional funds to commercialize its product candidates. The Company's cash requirements may vary materially from those now planned because of results of research and development, results of pre-clinical and clinical testing, responses to grant requests, relationships with strategic partners, changes in the focus and direction in the Company's research and development programs, competitive and technological advances, the regulatory process, and other factors. In any -6- of these circumstances, the Company may require substantially more funds than are currently available or than management intends to raise. The Company believes its existing unrestricted cash and cash equivalents, and the grants the Company has received or has been awarded and is awaiting disbursement of, will be sufficient to meet the Company's planned expenditures through at least the next twelve months, although there can be no assurance that the Company will not require additional funds. Management may seek to satisfy future funding requirements through public or private offerings of securities, by collaborative or other arrangements with pharmaceutical or biotechnology companies or from other sources. The Company's ability to continue as a going concern is dependent upon its ability to generate sufficient funds to meet its obligations as they become due and, ultimately, to obtain profitable operations. Management's plans for the forthcoming year, in addition to normal operations, include continuing their efforts to obtain additional equity and/or debt financing, and to obtain additional research grants and entering into research and development agreements with other entities. Principles of Consolidation - The consolidated financial statements include the accounts of Immtech International, Inc. and its wholly-owned subsidiaries (see Note 2). All intercompany balances and transactions have been eliminated. Cash and Cash Equivalents - The Company considers all highly liquid investments with a maturity of three months or less when purchased to be cash equivalents. Cash and cash equivalents consist of an amount on deposit at a bank and an investment in a money market mutual fund, stated at cost, which approximates fair value. Restricted Funds on Deposit - Restricted funds on deposit consist of cash in two accounts on deposit at a bank that is restricted for use in accordance with a clinical research subcontract agreement with The University of North Carolina at Chapel Hill and with Medicines for Malaria Venture ("MMV"). Concentration of Credit Risk - The Company maintains its cash in commercial banks. Balances on deposit are insured by the Federal Deposit Insurance Corporation ("FDIC") up to specified limits. Balances in excess of FDIC limits are uninsured. Investment - The Company accounts for its investment in NextEra Therapeutics, Inc. ("NextEra") on the equity method. As of March 31, 2003 and 2004, the Company owned approximately 28% of the issued and outstanding shares of NextEra common stock. The Company has recognized an equity loss in NextEra to the extent of the basis of its investment, and the investment balance is zero as of March 31, 2003 and 2004. Recognition of any investment income on the equity method by the Company for its investment in NextEra will occur only after NextEra has earnings in excess of previously unrecognized equity losses. Property and Equipment - Property and equipment are recorded at cost and depreciation and amortization are provided using the straight-line method over the estimated useful lives of the respective assets ranging from three to fifty years. -7- Land Use Rights - Land use rights represent an agreement by Lenton Fibre Optics Development Limited ("Lenton") to use land in the People's Republic of China for a period of 50 years and was being amortized over that period on a straight-line basis prior to the Super Insight transaction discussed in Note 2, resulting in the elimination of this agreement. Long-Lived Assets - The Company periodically evaluates the carrying value of its property and equipment. Long-lived assets are reviewed for impairment whenever events or changes in circumstances indicate that the carrying amount may not be recoverable. If the sum of the expected future undiscounted cash flows is less than the carrying amount of an asset, a loss is recognized for the asset and is measured by the difference between the fair value and the carrying value of the asset. Minority Interest - Minority interest represents the carryover basis of the 20% of Lenton not owned by the Company at the date of acquisition, plus equity in earnings or minus equity in losses from that date (see Note 2). Deferred Rental Obligation - Rental obligations with scheduled rent increases are recognized on a straight-line basis over the lease term. Revenue Recognition - Grants to perform research are the Company's primary source of revenue and are generally granted to support research and development activities for specific projects or drug candidates. Revenue related to grants to perform research and development is recognized as earned based on the performance requirements of the specific grant. Upfront cash payments from research and development grants are reported as deferred revenue until such time as the research and development activities covered by the grant are performed. Research and Development Costs - Research and development costs are expensed as incurred and include costs associated with research performed pursuant to collaborative agreements. Research and development costs consist of direct and indirect internal costs related to specific projects as well as fees paid to other entities that conduct certain research activities on behalf of the Company. Income Taxes - The Company accounts for income taxes using an asset and liability approach. Deferred income tax assets and liabilities are computed annually for differences between the financial statement and tax bases of assets and liabilities that will result in taxable or deductible amounts in the future based on enacted tax laws and rates applicable to the periods in which the differences are expected to affect taxable income. In addition, a valuation allowance is recognized if it is more likely than not that some or all of the deferred income tax assets will not be realized. A valuation allowance is used to offset the related net deferred income tax assets due to uncertainties of realizing the benefits of certain net operating loss and tax credit carryforwards and other deferred income tax assets. Net Income (Loss) Per Share - Net income (loss) per share is calculated in accordance with SFAS No. 128, "Earnings Per Share." Basic net income (loss) per share and diluted -8- net loss per share are computed by dividing net income (loss) attributable to common stockholders by the weighted average number of common shares outstanding. Diluted net income per share, when applicable, is computed by dividing net income attributable to common stockholders by the weighted average number of common shares outstanding increased by the number of potential dilutive common shares. Diluted net loss per share was the same as the basic net loss per share for the years ended March 31, 2002, 2003 and 2004. Potentially dilutive shares for common stock options and warrants and conversion of Series A, B, C and D Convertible Preferred Stock were not included in net income (loss) per share as their effect was antidilutive for each of the years then ended. Stock-Based Compensation - The Company has adopted the disclosure-only provisions of SFAS No. 123, "Accounting for Stock-Based Compensation," and applies Accounting Principles Board Opinion No. 25 and related interpretations in accounting for its employee stock option plans. During the years ended March 31, 2002, 2003 and 2004, the Company issued 95,750, 203,000 and 277,000 stock options, respectively, to certain employees and directors. If the Company had recognized compensation expense for the options granted during the years ended March 31, 2002, 2003, and 2004, consistent with the fair-value method prescribed by SFAS No. 123, net loss and net loss per share would have been changed to the pro forma amounts indicated below: 2002 2003 2004 Net loss attributable to common shareholders - as reported $ (4,261,045) $ (5,130,938) $(16,372,090) Add: stock-based compensation expense included in reported net loss 0 0 0 Deduct: total employee stock-based compensation expense determined under fair value method for all awards (270,329) (295,177) (1,205,881) ------------ ------------ ------------ Net loss attributable to common stockholders - pro forma $ (4,531,374) $ (5,426,115) $(17,577,971) ============ ============ ============ Basic and diluted net loss per share attributable to common stockholders - as reported $ (0.71) $ (0.78) $ (1.82) ============ ============ ============ Basic and diluted net loss per share attributable to common stockholders - pro forma $ (0.75) $ (0.83) $ (1.96) ============ ============ ============ The following weighted average assumptions were used for grants during the year ended March 31, 2002: 1) expected dividend yield of 0%, 2) risk-free interest rate of 5.0%, 3) expected volatility of 87%, and 4) expected option life of 7.1 years. The following weighted average assumptions were used for grants during the year ended March 31, 2003: 1) expected dividend yield of 0%, 2) risk-free interest rate of 3.8%, 3) expected volatility of 87%, and 4) expected option life of 9.5 years. The following weighted average assumptions were used for grants during the year ended March 31, 2004: 1) expected dividend yield of 0%, 2) risk-free interest rate of 4.3%, 3) expected volatility of 113%, and 4) expected option life of 10 years. -9- The Black-Scholes option valuation model was developed for use in estimating the fair value of traded options that have no vesting restrictions and are fully transferable. In addition, option valuation models require the input of highly subjective assumptions, including the expected stock price volatility. Because the Company's options have characteristics significantly different from traded options, and because changes in the subjective input assumptions can materially affect the fair value estimate, in the opinion of management, the existing models do not necessarily provide a reliable single value of its options and may not be representative of the future effects on reported net income (loss) or the future stock price of the Company. The weighted average estimated fair value of employee stock options granted during the years ended March 31, 2002, 2003 and 2004 was $5.46, $2.15 and $18.23, respectively. For purposes of pro forma disclosure, the estimated fair value of the options is amortized to expense over the options' vesting period. Fair Value of Financial Instruments - The Company believes that the carrying amount of its financial instruments (cash and cash equivalents, restricted funds on deposit, accounts payable and accrued expenses) approximates the fair value of such instruments as of March 31, 2003 and 2004 based on the short-term nature of the instruments. Segment Reporting - The Company is a development stage pharmaceutical company that operates as one segment. Comprehensive Loss - There were no cumulative differences between comprehensive loss and net loss for the years presented. Use of Estimates - The preparation of financial statements in conformity with accounting principles generally accepted in the United States of America requires management to make estimates and assumptions that affect the reported amounts of assets and liabilities and disclosure of contingent assets and liabilities at the date of the financial statements and the reported amounts of revenues and expenses during the reporting period. Actual results could differ from those estimates. 2. EXCHANGE OF OWNERSHIP INTERESTS On November 28, 2003, the Company entered into a share purchase agreement and deed of indemnity (the "Share Purchase Agreement") as related to the shares in Super Insight Limited ("Super Insight") and a share purchase agreement and deed of indemnity as related to the shares in Super Insight and Immtech Hong Kong Limited (the "Allonge") with Mr. Chan Kon Fung ("Mr. Chan"), Lenton, Super Insight and Immtech Hong Kong Limited. Pursuant to the terms of the Share Purchase Agreement and the Allonge, Immtech purchased (i) from Mr. Chan 100% of the outstanding shares of Super Insight and its wholly-owned subsidiary, subsequently named Immtech Life Science Limited ("Immtech Life Science") and (ii) from Lenton, 100% of Lenton's interest in Immtech Hong Kong. As payment for the shares of Super Insight and Immtech Hong Kong, Immtech transferred to Mr. Chan its 80% interest in Lenton and $400,000 in cash. -10- Immtech Life Science has ownership of two floors of a newly-constructed building located in the Futian Bounded Zone, Shenzhen, in the People's Republic of China through May 2051, which is classified as leasehold improvements in the accompanying March 31, 2004 consolidated balance sheet. This transaction resulted in the surrender of the Company's ownership interest in Lenton and the consolidation of the Company's wholly-owned subsidiary, Super Insight. The primary asset of Lenton was land-use rights in China and the primary assets of Super Insight are leasehold improvements consisting of two floors of the building described above. This transaction has been accounted for as a like-kind exchange of similar assets. Accordingly, this transaction did not impact the Company's consolidated statement of operations. 3. RECAPITALIZATION, PRIVATE PLACEMENTS AND INITIAL PUBLIC OFFERING On July 24, 1998 (the "Effective Date"), the Company completed a recapitalization (the "Recapitalization") pursuant to which, among other items: (i) the Company's debt holders converted approximately $3,151,000 in stockholder advances, notes payable and related accrued interest and accounts payable outstanding immediately prior to the Effective Date into 604,978 shares of common stock and approximately $203,000 in cash (see Note 10); and (ii) the Company's Series A Redeemable Preferred stockholders converted 1,794,550 shares of Series A Redeemable Preferred Stock issued and outstanding immediately prior to the Effective Date into 578,954 shares of common stock (see Note 10); (iii) the Company's Series B Redeemable Preferred stockholders converted 1,600,000 shares of Series B Redeemable Preferred Stock issued and outstanding immediately prior to the Effective Date into 616,063 shares of common stock (see Note 10). Contemporaneously with the completion of the Recapitalization, the Company issued and sold 575,000 shares of common stock for $1.74 per share, or aggregate consideration to the Company of $1,000,000 to certain accredited investors under a private placement offering. For services and expenses involved with this Recapitalization, the placement agent, New China Hong Kong Securities Limited ("NCHK") received $50,000 and warrants to purchase 75,000 shares of the Company's common stock at $.10 per share. On May 17, 1999, NCHK exercised their warrants. For advisory services in this transaction, RADE Management Corporation ("RADE") received warrants to purchase 225,000 shares of the Company's common stock at $.10 per share. On April 22, 1999, the warrant agreement with RADE was amended to increase the exercise price from $.10 per share to $6.47 per share. The warrants expire July 24, 2004 (see Note 7). The private placement offering resulted in net proceeds of approximately $831,000. RADE leases an office facility which is occupied by both the Company and RADE. The office space is paid for by Immtech on RADE's behalf (see Note 9). During the years ended March 31, 2002, 2003, and 2004, the Company paid approximately $106,000, $106,000 and $121,000 respectively, for the use of the facility. In addition, during the year ended March 31, 2002, approximately $18,000, was paid to RADE as reimbursement for certain administrative expenses paid on behalf of the Company. -11- On April 26, 1999, the Company issued 1,150,000 shares of common stock through an initial public stock offering resulting in net proceeds of approximately $9,173,000. Costs incurred of approximately $513,000 were netted with the proceeds of the offering. The underwriters received warrants to purchase 100,000 additional shares of common stock at $16.00 per share (see Note 7). The warrants expired on April 25, 2004. On December 8, 2000, the Company completed a private placement offering which raised approximately $4,306,000 of additional equity capital through the issuance of 584,250 shares of common stock. In February 2002, the Company completed private placement offerings which raised approximately $3,849,000 of additional equity capital (net of approximately $154,000 of cash offering costs) through the issuance of 160,100 shares of Series A Convertible Preferred Stock and warrants to purchase 400,250 shares of the Company's common stock at an exercise price of $6.00 per share. The warrants expire five years from the date of grant (see Note 7). In September and October 2002, the Company completed private placement offerings which raised approximately $1,859,000 of additional equity capital (net of approximately $59,000 of cash offering costs) through the issuance of 76,725 shares of Series B Convertible Preferred Stock and warrants to purchase 191,812 shares of the Company's common stock at an exercise price of $6.125 per share. The warrants expire five years from the date of grant (see Note 7). In June 2003, the Company completed private placement offerings which raised approximately $2,845,000 of additional equity capital (net of approximately $289,000 of cash offering costs) through the issuance of 125,352 shares of Series C Convertible Preferred Stock. Total cash and noncash offering costs with respect to the issuance of the Series C Convertible Preferred Stock was approximately $1,685,000. In January 2004, the Company completed private placement offerings which raised approximately $4,571,000 of additional equity capital (net of approximately $429,000 of cash offering costs) through the issuance of 200,000 shares of Series D Convertible Preferred Stock and warrants to purchase 200,000 shares of the Company's common stock at an exercise price of $16.00 per share. The warrants expire five years from the date of grant (see Note 7). 4. INVESTMENT IN NEXTERA THERAPEUTICS, INC. On July 8, 1998, the Company, together with Franklin Research Group, Inc. ("Franklin") and certain other parties, formed NextEra Therapeutics, Inc. ("NextEra") to develop therapeutic products for treating cancer and related diseases. The Company and Franklin have a research and funding agreement with NextEra in which Franklin provided funding of $1,350,000 to NextEra to fund the scale-up of manufacturing for and initiation of certain clinical trials of NextEra's product candidates. The Company contributed its rmCRP technology as well as use of its current laboratory facilities for shares of common stock of NextEra. During the year ended March 31, 2000, the Company advanced -12- $135,000 to NextEra to fund its operations. The Company's advance to NextEra was expensed during the year ended March 31, 2000. The Company did not advance any funds to NextEra during the years ended March 31, 2002, 2003 and 2004. NextEra funded the operation of the Company's primary facility, including certain salaries related to work on rmCRP, rent and overhead associated with the project from July 1998 through December 1999. Since January 1, 2000, NextEra has funded only their own compensation expenses, as they stopped funding the Company's primary facility and any associated overhead. In addition, NextEra has funded and is required to fund the cost of maintaining and defending the patents that are part of the intellectual property transferred to NextEra by the Company. NextEra has incurred accumulated losses of approximately $2,905,000 since inception (July 8, 1998) through March 31, 2004. NextEra is expected to continue to incur significant losses during the next several years. In addition, as of March 31, 2004, NextEra's current liabilities exceeded its current assets by approximately $361,000 and NextEra had a stockholders' equity of approximately $147,000. As of March 31, 2003 and 2004, the Company owned approximately 28% of the issued and outstanding shares of NextEra common stock. On April 27, 2000, Franklin filed a complaint against the Company in the United States District Court for the Southern District of Ohio, Eastern Division alleging fraud, negligent misrepresentation and breach of the implied covenant of good faith and fair dealing in connection with the research and funding agreement entered into between Franklin, the Company and NextEra. The complaint sought compensatory damages, unquantified punitive damages, attorneys' fees, costs and expenses. On March 23, 2001, Franklin voluntarily dismissed its complaint against the Company and together with NextEra filed a new complaint in the Court of Common Pleas, Franklin County, Ohio alleging fraud, negligent misrepresentation and breach of the implied covenant of good faith and fair dealing in connection with the research and funding agreement entered into between Franklin, the Company and NextEra. In addition, NextEra alleged the Company tortuously interfered with an employment agreement between NextEra and the chief scientific officer of NextEra. The complaint sought compensatory damages in excess of $25,000, unquantified punitive damages, attorneys' fees, costs and expenses. On May 25, 2001, the case was dismissed without prejudice by the Court of Common Pleas, Franklin County, Ohio. The Company is currently in negotiations with Franklin and its designees to resolve certain issues, including the possible restructuring of the joint venture and relationship with NextEra to better position NextEra in its fund-raising efforts, and increasing the Company's ownership interest in NextEra as consideration for services provided to NextEra, expenses the Company previously incurred on behalf of NextEra and funds previously advanced to NextEra. NextEra's ability to continue as a going concern is dependent upon its ability to generate sufficient funds to meet its obligations as they become due and, ultimately, to obtain profitable operations. NextEra's financial plans for the forthcoming year include continuing efforts to obtain additional equity financing. -13- The Company has recognized an equity loss in NextEra to the extent of the basis of its investment. Future recognition of any investment income on the equity method by the Company for its investment in NextEra will occur only after NextEra has earnings in excess of previously unrecognized equity losses. As of March 31, 2003 and 2004, the Company's net investment in NextEra is zero. The following is summarized financial information for NextEra as of March 31, 2002, 2003, and 2004 and for the years then ended: 2002 2003 2004 Current assets $ 309,000 $ 281,000 $ 281,000 Noncurrent assets 642,000 566,000 508,000 Current liabilities: Advances from Franklin 71,000 -- -- Advances from the Company 135,000 135,000 135,000 Advances from other shareholders 40,000 88,000 183,000 Other 525,000 353,000 324,000 Stockholders' equity 117,000 271,000 147,000 Revenues 46,000 -- -- Net (loss) income (796,000) 91,000 (124,000) Net loss (inception to date) (2,872,000) (2,781,000) (2,905,000) 5. PROPERTY AND EQUIPMENT Property and equipment consist of the following as of March 31, 2003 and 2004: 2003 2004 Land use rights $3,501,522 Research and laboratory equipment 474,455 $ 477,609 Furniture and office equipment 157,824 169,069 Leasehold improvements 28,525 3,587,519 ---------- ---------- Property and equipment - at cost 4,162,326 4,234,197 Less accumulated depreciation and amortization 557,670 623,983 ---------- ---------- Property and equipment - net $3,604,656 $3,610,214 ========== ========== 6. INCOME TAXES The Company accounts for income taxes using an asset and liability approach which generally requires the recognition of deferred income tax assets and liabilities based on the expected future income tax consequences of events that have previously been recognized in the Company's financial statements or tax returns. In addition, a valuation allowance is recognized if it is more likely than not that some or all of the deferred income tax assets will not be realized. A valuation allowance is used to offset the related net deferred income tax assets due to uncertainties of realizing the benefits of certain net operating loss and tax credit carryforwards and other deferred income tax assets. -14- The Company has no significant deferred income tax liabilities. Significant components of the Company's deferred income tax assets are as follows: March 31, -------------------------------- 2003 2004 Deferred income tax assets: Federal net operating loss carryforwards $ 11,437,000 $ 14,566,000 State net operating loss carryforwards 1,486,000 1,972,000 Federal income tax credit carryforwards 701,000 750,000 Deferred revenue 991,000 710,000 ------------ ------------ Total deferred income tax assets 14,615,000 17,998,000 ------------ ------------ Valuation allowance (14,615,000) (17,998,000) ------------ ------------ Net deferred income taxes recognized in the accompanying balance sheets $ 0 $ 0 ============ ============ As of March 31, 2004, the Company had federal net operating loss carryforwards of approximately $42,840,000 which expire from 2006 through 2024. The Company also has approximately $41,092,000 of state net operating loss carryforwards as of March 31, 2004, which expire from 2009 through 2024, available to offset future taxable income for state (primarily Illinois) income tax purposes. Because of "change of ownership" provisions of the Tax Reform Act of 1986, approximately $920,000 of the Company's net operating loss carryforwards for federal income tax purposes are subject to an annual limitation regarding utilization against taxable income in future periods. As of March 31, 2004, the Company had federal income tax credit carryforwards of approximately $750,000 which expire from 2008 through 2024. A reconciliation of the provision for income taxes (benefit) at the federal statutory income tax rate to the effective income tax rate follows: Years Ended March 31, ---------------------------- 2002 2003 2004 Federal statutory income tax rate (34.0)% (34.0)% (34.0)% State income taxes (4.8) (4.8) (4.8) Non-deductible compensation and expenses 4.9 9.0 0.0 Benefit of federal and state net operating loss and tax credit carryforwards and other deferred income tax assets not recognized 33.9 29.8 38.8 ----- ----- ----- Effective income tax rate 0.0% 0.0% 0.0% ----- ----- ----- 7. STOCKHOLDERS' EQUITY On January 7, 2004, the shareholders of the Company approved an increase in the number of authorized common stock from 30 million to 100 million shares. -15- Series A Convertible Preferred Stock - On February 14, 2002, the Company filed a Certificate of Designation with the Secretary of State of the State of Delaware designating 320,000 shares of the Company's 5,000,000 authorized shares of preferred stock as Series A Convertible Preferred Stock, $0.01 par value, with a stated value of $25.00 per share. Dividends accrue at a rate of 6.0% per annum on the $25.00 stated value per share and are payable semi-annually on April 15, and October 15 of each year while the shares are outstanding. The Company has the option to pay the dividend either in cash or in equivalent shares of common stock, as defined. Included in the carrying value of the Series A Convertible Preferred Stock in the accompanying condensed consolidated balance sheets is $55,250 and $98,005 of accrued preferred stock dividends at March 31, 2004 and 2003, respectively. Each share of Series A Convertible Preferred Stock may be converted by the holder at any time into shares of the Company's common stock at a conversion rate determined by dividing the $25.00 stated value, plus any accrued and unpaid dividends (the "Liquidation Price"), by a $4.42 conversion price (the "Conversion Price A"), subject to certain antidilution adjustments, as defined in the Certificate of Designation. During the year ended March 31, 2001, the Company issued 160,100 shares of Series A Convertible Preferred Stock for net proceeds of $3,849,000 (less cash offering costs of approximately $184,000). On October 15, 2003, the Company issued 4,010 shares of common stock and paid $296 in lieu of fractional common shares as dividends on the preferred shares and on April 15, 2003, the Company issued 23,316 shares of common stock and paid $96 in lieu of fractional common shares as dividends on the preferred shares. On October 15, 2002, the Company issued 28,959 shares of common stock and paid $64 in lieu of fractional common shares as dividends on the preferred shares and on April 15, 2002, the Company issued 8,249 shares of common stock and paid $166 in lieu of fractional common shares as dividends on the preferred shares. During the years ended March 31, 2004 and 2003, certain preferred stockholders converted 62,000 and 17,300 shares of Series A Convertible Preferred Stock, including accrued dividends, for 353,667 and 99,105 shares of common stock, respectively. The Company may require that any or all outstanding shares of Series A Convertible Preferred Stock be converted into shares of the Company's common stock. The number of shares of common stock to be received by the holders of the Series A Convertible Preferred Stock upon a mandatory conversion by the Company is determined by (i) dividing the Liquidation Price by the Conversion Price A, provided that the closing bid price for the Company's common stock exceeds $9.00 for 20 consecutive trading days within 180 days prior to notice of conversion, as defined, or (ii) if the requirements of (i) are not met, the number of shares of common stock is determined by dividing 110% of the Liquidation Price by the Conversion Price. During the year ended March 31, 2004, the closing price of the Company's common stock did exceed $9 per share for 20 consecutive days. The Conversion Price is subject to certain antidilution adjustments, as defined in the Certificate of Designation. The Company may at any time, upon 30 day's notice, redeem any or all outstanding shares of the Series A Convertible Preferred Stock by payment of the Liquidation Price to the holder of such shares, provided that the holder does not convert the Series A Convertible Preferred Stock into shares of Common Stock during the 30 day period. -16- Each issued and outstanding share of Series A Convertible Preferred Stock shall be entitled to 5.6561 votes with respect to any and all matters presented to the stockholders of the Company for their action or consideration. Except as provided by law or by the provisions establishing any other series of preferred stock, Series A Convertible Preferred stockholders and holders of any other outstanding preferred stock shall vote together with the holders of common stock as a single class. Series B Convertible Preferred Stock - On September 5, 2002, the Company filed a Certificate of Designation with the Secretary of State of the State of Delaware designating 240,000 shares of the Company's 5,000,000 authorized shares of preferred stock as Series B Convertible Preferred Stock, $0.01 par value, with a stated value of $25.00 per share. Dividends accrue at a rate of 8.0% per annum on the $25.00 stated value per share and are payable semi-annually on April 15 and October 15 of each year while the shares are outstanding. The Company has the option to pay the dividend either in cash or in equivalent shares of common stock, as defined. Included in the carrying value of the Series B Convertible Preferred Stock in the accompanying consolidated balance sheets is $17,968 and $51,842 of accrued preferred stock dividends as of March 31, 2004 and 2003, respectively. Each share of Series B Convertible Preferred Stock may be converted by the holder at any time into shares of the Company's common stock at a conversion rate determined by dividing the $25.00 stated value, plus any accrued and unpaid dividends (the "Liquidation Price"), by a $4.00 conversion price (the "Conversion Price B"), subject to certain antidilution adjustments, as defined in the Certificate of Designation. During the year ended March 31, 2003, the Company issued 76,725 shares of Series B Convertible Preferred Stock for net proceeds of $1,859,000 (net of cash offering costs of approximately $59,000). On October 15, 2003, the Company issued 1,130 shares of common stock and paid $139 in lieu of fractional common shares as dividends on the preferred shares and on April 15, 2003, the Company issued 11,049 shares of common stock and paid $17 in lieu of fractional common shares as dividends on the preferred shares. On October 15, 2002, the Company issued 2,658 shares of common stock and paid $17 in lieu of fractional common shares as dividends on the preferred shares. During the years ended March 31, 2004 and 2003, certain preferred stockholders converted 36,800 and 20,000 shares of Series B Convertible Preferred stock, including accrued dividends, for 232,851 and 129,343 shares of common stock, respectively. The Company may require that any or all outstanding shares of Series B Convertible Preferred Stock be converted into shares of the Company's common stock. The number of shares of common stock to be received by the holders of the Series B Convertible Preferred Stock upon a mandatory conversion by the Company is determined by (i) dividing the Liquidation Price by the Conversion Price B, provided that the closing bid price for the Company's common stock exceeds $9.00 for 20 consecutive trading days within 180 days prior to notice of conversion, as defined, or (ii) if the requirements of (i) are not met, the number of shares of common stock is determined by dividing 110% of the Liquidation Price by the Conversion Price B. During the year ended March 31, 2004, the closing price of the Company's common stock did exceed $9 per share for 20 consecutive days. The Conversion Price B is subject to certain antidilution adjustments, as defined in the Certificate of Designation. -17- The Company may at any time, upon 30-day notice, redeem any or all outstanding shares of the Series B Convertible Preferred Stock by payment of the Liquidation Price to the holder of such shares, provided that the holder does not convert the Series B Convertible Preferred Stock into shares of common stock during the 30 day period. Each issued and outstanding share of Series B Convertible Preferred Stock shall be entitled to 6.25 votes (subject to adjustment for dilution) with respect to any and all matters presented to the stockholders of the Company for their action or consideration. Except as provided by law or by the provisions establishing any other series of preferred stock, Series B Convertible Preferred stockholders and holders of any other outstanding preferred stock shall vote together with the holders of common stock as a single class. Series C Convertible Preferred Stock - On June 6, 2003, the Company filed a Certificate of Designation with the Secretary of State of the State of Delaware designating 160,000 shares of the Company's 5,000,000 authorized shares of preferred stock as Series C Convertible Preferred Stock, $0.01 par value, with a stated value of $25.00 per share. Dividends accrue at a rate of 8.0% per annum on the $25.00 stated value per share and are payable semi-annually on April 15 and October 15 of each year while the shares are outstanding. The Company has the option to pay the dividend either in cash or in equivalent shares of common stock, as defined. Included in the carrying value of the Series C Convertible Preferred Stock in the accompanying March 31, 2004 consolidated balance sheet is $66,586 of accrued preferred stock dividends. Each share of Series C Convertible Preferred Stock may be converted by the holder at any time into shares of the Company's common stock at a conversion rate determined by dividing the $25.00 stated value, plus any accrued and unpaid dividends (the "Liquidation Price"), by a $4.42 conversion price (the "Conversion Price C"), subject to certain antidilution adjustments, as defined in the Certificate of Designation. During the year ended March 31, 2004, the Company issued 125,352 shares of Series C Convertible Preferred Stock for net proceeds of $2,845,000 (net of approximately $289,000 of cash offering costs). Total cash and noncash offering costs with respect to the issuance of the Series C Convertible Preferred Stock was approximately $1,685,000. The preferred shares issued have an embedded beneficial conversion feature based on the market value on the day of issuance and the price of conversion. The beneficial conversion was equal to approximately $1,120,000 and was accounted for as a deemed dividend during the year ended March 31, 2004. On October 15, 2003, the Company issued 4,893 shares of common stock and paid $594 in lieu of fractional common shares as dividends on the preferred shares. During the year ended March 31, 2004, certain preferred stockholders converted 53,048 shares of Series C Convertible Preferred Stock, including accrued dividends, for 301,299 shares of common stock. The Company may at any time after May 31, 2004, require that any or all outstanding shares of Series C Convertible Preferred Stock be converted into shares of the Company's common stock, provided that the shares of common stock into which the Series C Convertible Preferred Stock are convertible are registered pursuant to an effective registration statement, as defined. The number of shares of common stock to be received by the holders of the Series C Convertible Preferred Stock upon a mandatory conversion by the Company is determined by (i) dividing the Liquidation Price by the Conversion Price C provided that the closing bid price for the Company's common stock exceeds $9.00 for 20 consecutive trading days within 180 days prior to notice of conversion, as defined, or (ii) if the requirements of (i) are not met, the number of shares -18- of common stock is determined by dividing 110% of the Liquidation Price by the Conversion Price C. During the year ended March 31, 2004, the closing price of the Company's common stock did exceed $9 per share for 20 consecutive days. The Conversion Price C is subject to certain antidilution adjustments, as defined in the Certificate of Designation. The Company may at any time, upon 30 day notice, redeem any or all outstanding shares of the Series C Convertible Preferred Stock by payment of the Liquidation Price to the holder of such shares, provided that the holder does not convert the Series C Convertible Preferred Stock into shares of common stock during the 30 day period. Each issued and outstanding share of Series C Convertible Preferred Stock shall be entitled to 5.6561 votes (subject to adjustment for dilution) with respect to any and all matters presented to the stockholders of the Company for their action or consideration. Except as provided by law or by the provisions establishing any other series of preferred stock, Series C Convertible Preferred stockholders and holders of any other outstanding preferred stock shall vote together with the holders of common stock as a single class. Series D Convertible Preferred Stock - On January 15, 2004, the Company filed a Certificate of Designation with the Secretary of State of the State of Delaware designating 200,000 shares of the Company's 5,000,000 authorized shares of preferred stock as Series D Convertible Preferred Stock, $0.01 par value, with a stated value of $25.00 per share. Dividends accrue at a rate of 6.0% per annum on the $25.00 stated value per share and are payable semi-annually on April 15 and October 15 of each year while the shares are outstanding. The Company has the option to pay the dividend either in cash or in equivalent shares of common stock, as defined. Included in the carrying value of the Series D Convertible Preferred Stock in the accompanying consolidated balance sheet is $56,712 of accrued preferred stock dividends as of March 31, 2004. Each share of Series D Convertible Preferred Stock may be converted by the holder at any time into shares of the Company's common stock at a conversion rate determined by dividing the $25.00 stated value, plus any accrued and unpaid dividends (the "Liquidation Price"), by a $9.00 conversion price (the "Conversion Price D"), subject to certain antidilution adjustments, as defined in the Certificate of Designation. During the year ended March 31, 2004, the Company issued 200,000 shares of Series D Convertible Preferred Stock for net proceeds of approximately $4,571,000 (net of approximately $429,000 of cash offering costs). In connection with the Series D Preferred Stock offering, the Company entered into a Finder's Agreement with Ace Noble Holdings Limited (the "Finder") to identify and introduce qualified leads, increase financial market awareness in the Company and to assist the Company in raising funds. As consideration for services to be performed under this agreement, the Company was obligated to pay a cash fee of 8% of funds invested in Immtech's Series D Preferred Stock by Non-U.S. persons prior to January 23, 2004 by investors introduced by the Finder and expenses not to exceed $36,000. During the year ended March 31, 2004, fees of $350,000 and expenses of $36,000 were paid with respect to this agreement, which are included as part of the $429,000 of cash offering costs. -19- The Company may at any time after January 1, 2005, require that any or all outstanding shares of Series D Convertible Preferred Stock be converted into shares of the Company's common stock, provided that the shares of common stock into which the Series D Convertible Preferred Stock are convertible are registered pursuant to an effective registration statement, as defined. The number of shares of common stock to be received by the holders of the Series D Convertible Preferred Stock upon a mandatory conversion by the Company is determined by (i) dividing the Liquidation Price by the Conversion Price D provided that the closing bid price for the Company's common stock exceeds $18.00 for 20 consecutive trading days within 180 days prior to notice of conversion, as defined, or (ii) if the requirements of (i) are not met, the number of shares of common stock is determined by dividing 110% of the Liquidation Price by the Conversion Price D. The Conversion Price D is subject to certain antidilution adjustments, as defined in the Certificate of Designation. The Company may at any time, upon 30-day notice, redeem any or all-outstanding shares of the Series D Convertible Preferred Stock by payment of the Liquidation Price to the holder of such shares, provided that the holder does not convert the Series D Convertible Preferred Stock into shares of common stock during the 30 day period. Each issued and outstanding share of Series D Convertible Preferred Stock shall be entitled to 2.7778 votes (subject to adjustment for dilution) with respect to any and all matters presented to the stockholders of the Company for their action or consideration. Except as provided by law or by the provisions establishing any other series of preferred stock, Series D Convertible Preferred stockholders and holders of any other outstanding preferred stock shall vote together with the holders of common stock as a single class. Common Stock - On June 28, 2002, the Company entered into a Finder's Agreement with an individual to develop and qualify potential strategic partners for the purpose of testing and/or the commercialization of Company products in China. As consideration for entering into the agreement, the individual received 150,000 shares of the Company's common stock and the Company recognized approximately $757,500 as a general and administrative expense based on the estimated fair value of the shares issued. On July 31, 2002, the Company entered into a one-year agreement with The Gabriele Group. L.L.C. ("Gabriele") for assistance to be provided by Gabriele to the Company with respect to management consulting, strategic planning, public relations and promotions. As compensation for these services, the Company granted Gabriele 40,000 shares of the Company's common stock and the Company recognized approximately $187,600 as a general and administrative expense during the year ended March 31, 2003, based on the fair value of the shares on the date issued. The Company also granted Gabriele warrants to purchase 30,000 shares of the Company's common stock at $6.00 per share. These warrants vest when the price of the Company's common stock reaches certain milestones. During the year ended March 31, 2004, the Company recognized general and administrative expenses of approximately $247,000 because the prescribed milestones had been reached with respect to 20,000 of the warrants to purchase the Company's stock. The remaining 10,000 warrants may vest in the future if certain milestones are achieved. This expense was recorded based on the estimated fair value of the warrants using the Black-Scholes option valuation model. -20- On March 21, 2003, the Company entered into media production agreements with Winmaxmedia, an operating division of Winmax Trading Group, Inc. ("Winmax"), to produce materials to be used in connection with equity fundraising efforts. As consideration for services to be performed under the agreement, the Company issued 100,000 shares of its common stock and paid approximately $100,000 of cash during the year ended March 31, 2003, which was recorded as deferred offering costs within other current assets on the accompanying March 31, 2003 consolidated balance sheet. On March 21, 2003, the Company entered into an Investor Relations Agreement with Fulcrum Holdings of Australia, Inc. ("Fulcrum") for financial consulting services and public relations management to be provided over a 12-month period. As consideration for services to be performed under the agreement, the Company is to issue to Fulcrum 100,000 shares of common stock and warrants to purchase 350,000 shares of common stock at prices ranging from $6.00 to $15.00 per share. During the year ended March 31, 2004, the common shares and warrants were issued, and the related expense was recognized, on a pro-rata basis over the contract period. During the years ended March 31, 2003 and 2004, 8,333 and 91,667 common shares were issued and general and administrative expenses of $37,290 and $1,031,756, respectively, were recorded based on the market value of the common shares on the date of issuance. Also during the years ended March 31, 2003 and 2004, warrants to purchase 29,167 and 320,833 shares of common stock were issued and general and administrative expenses of $51,835 and $1,748,411, respectively, were recorded based on the estimated fair value of the warrants using the Black-Scholes option valuation model. On March 21, 2003, the Company entered into a Finder's Agreement with Wyndham Associates Limited ("Wyndham") to identify potential strategic partners and assist in the raising of equity financing. As consideration for services to be performed under the agreement, the Company was obligated to issue 220,000 shares of common stock. The agreement further provided that Wyndham would receive a cash fee for any additional equity investments by investors introduced by Wyndham. During the year ended March 31, 2004, 220,000 common shares were issued and non-cash offering costs of $1,397,000 were recorded based on the market value of the Company's common stock on the date of issuance. On July 25, 2003, the Company entered into a consulting agreement with Fulcrum to identify and negotiate with stock exchanges to list the common stock of the Company and to assist the Company to prepare applications to list the common stock of the Company on a stock exchange. As consideration for services under this agreement, upon the listing of the Company's common stock on a stock exchange, the Company would issue to Fulcrum 100,000 shares of common stock. On August 11, 2003, the Company's common stock was listed on the American Stock Exchange. Accordingly, the Company issued 100,000 shares of its common stock to Fulcrum, resulting in the recognition of general and administrative expenses of $1,400,000 during the year ended March 31, 2004, based on the market value of the Company's common stock on the date of issuance. -21- In September 2003, the Company entered into a separate Finder's Agreement with Wyndham to identify potential strategic partners and assist in the private placements of debt, equity and/or warrants through December 2003. As consideration for services to be performed under this agreement, a cash fee equal to 8.0% of funds received by the Company from investors introduced by Wyndham, is due at the closing date of the respective private placement. The Company also paid a retainer of $160,000 to Wyndham. In the event that investors introduced by Wyndham did not subscribe to invest at least $20,000,000, the $160,000 retainer was to be returned to the Company. The minimum subscription amount of $20,000,000 was not achieved prior to December 31, 2003 and the $160,000 has not yet been repaid to the Company; instead it was written-off as a charge to general and administrative expenses during the year ended March 31, 2004. On July 16, 2003, the Company entered into a consulting agreement with David Tat-Koon Shu for services to assist the Company with the formation of a subsidiary and to gain regulatory approvals to enter into clinical trials in China. As compensation for these services, Mr. Shu was granted 10,000 shares of the Company's common stock and a general and administrative expense of $62,900 was recorded during the year ended March 31, 2004 based on the market value of the common stock on the date of issuance. Common Stock Options - On October 12, 2000, the Company's stockholders approved the issuance of options to purchase shares of common stock to certain employees and other nonemployees who have been engaged to assist the Company in various research and administrative capacities as part of the 2000 Stock Incentive Plan. The 2000 Stock Incentive Plan provides for the issuance of up to 350,000 shares of common stock in the form of incentive stock options and non-qualified stock options. At the stockholders meeting held November 15, 2002, the stockholders approved an amendment to the 2000 Stock Incentive Plan to increase the number of shares of common stock reserved for issuance from 350,000 shares to 1,100,000 shares. Expiring stock options which were issued under the 2000 Stock Incentive Plan are available for reissuance. During the year ended March 31, 2004, there were 8,500 options previously granted under the 2000 Stock Incentive Plan that expired and are available to be reissued. The incentive stock options must be granted at a price at least equal to fair market value at the date of grant. The Company has granted options to purchase common stock to individuals who have contributed to the Company in various capacities. The options contain various provisions regarding vesting periods and expiration dates. The options generally vest over periods ranging from 0 to 4 years and expire after five or ten years. As of March 31, 2004, there were a total of 340,250 shares available for grant. Options Granted to Nonemployees - During the year ended March 31, 2002, the Company issued options to purchase 12,000 shares of common stock to nonemployees and recognized expense of approximately $332,000 related to such options and certain other options issued in prior years which vest over a four-year service period. During the year ended March 31, 2003, the Company issued options to purchase 22,000 shares of common stock to nonemployees (of which options to purchase 5,000 shares did not vest) and recognized expense of approximately $243,000 related to such options and certain -22- other options issued in prior years which vest over a four year service period. During the year ended March 31, 2004, the Company issued options to purchase 22,000 shares of common stock to nonemployees and recognized expense of approximately $267,000 related to such options and certain other options issued in prior years which vest over a four year service period. The expense was determined based on the estimated fair value of the options using the Black-Scholes option valuation model and assumptions regarding volatility of the Company's common stock, risk-free interest rates, and life of the option of the Company's common stock all at the date such options were issued. The activity during the years ended March 31, 2002, 2003 and 2004 for the Company's stock options is summarized as follows: Weighted Number of Stock Options Average Shares Price Range Exercise Price Outstanding as of March 31, 2001 466,136 $0.34-11.50 $ 4.43 Granted 107,750 4.75-10.00 7.16 Exercised (51,214) 0.34- 0.59 0.38 Expired (14,194) 0.34-11.50 1.91 -------- ----------- ------ Outstanding as of March 31, 2002 508,478 0.34-11.50 5.48 Granted 225,000 2.25-4.75 2.75 Exercised (217) 0.59 0.59 Expired (34,787) 0.59-10.50 7.72 -------- ----------- ------ Outstanding as of March 31, 2003 698,474 0.34-11.50 4.49 Granted 299,000 6.08-21.66 17.80 Exercised (26,400) 0.46-11.50 2.57 Expired (8,500) 2.55-11.50 9.56 -------- ----------- ------ Outstanding as of March 31, 2004 962,574 0.34-21.66 8.63 ======== =========== ====== Exercisable as of March 31, 2002 340,186 $0.34-11.50 3.86 Exercisable as of March 31, 2003 415,709 0.34-11.50 4.52 Exercisable as of March 31, 2004 567,838 0.34-21.66 6.02 The following table summarizes information about stock options outstanding as of March 31, 2004: Options Outstanding Options Exercisable ------------------------------------------ ------------------------- Weighted Average Weighted Weighted Range Remaining Average Average of Exercise Shares Contractual Exercise Shares Exercise Prices Outstanding Life-Years Price Exercisable Price $0.34-0.46 152,634 2.87 $ 0.44 152,634 $ 0.44 1.74-2.55 257,190 6.56 2.37 139,538 2.23 4.42-4.75 73,000 3.06 4.73 52,503 4.72 6.08-11.50 202,750 5.26 10.38 180,142 10.68 14.29-21.66 277,000 9.63 18.71 43,021 20.16 ------- ----- ------ ------- ------- 962,574 5.07 $ 8.63 567,838 $ 6.02 ======= ===== ====== ======= ======= -23- Warrants - For advisory services in connection with the Recapitalization (see Note 3), RADE received warrants to purchase 225,000 shares of the Company's common stock at $.10 per share. On April 22, 1999, the warrant agreement with RADE was amended to increase the exercise price from $.10 per share to $6.47 per share. The warrants expire July 24, 2004. On October 12, 1998, RADE received warrants to purchase 750,000 shares of the Company's common stock at $.10 per share. On April 22, 1999, the warrant agreement was amended to increase the exercise price from $.10 per share to $6.47 per share. The warrants were issued as compensation for management consulting, market analysis and strategic advisory services performed from July 1998 through December 1998. The warrants expire October 12, 2004. In connection with an initial public offering, the underwriters received warrants to purchase 100,000 additional shares of common stock at $16.00 per share. The warrants expired on April 25, 2004. On July 31, 2000, the Company entered into an agreement with the principals of Stonegate Securities, Inc. ("Stonegate") for assistance by Stonegate in connection with raising additional equity capital for the consideration of warrants to purchase 200,000 shares of the Company's common stock. Pursuant to a notice of termination of the agreement dated December 8, 2000, 100,000 of the warrants shall not vest. The remaining 100,000 warrants expire on July 31, 2005 and have an exercise price of $12.06 per share. The Company recorded a general and administrative expense of $866,000 during the year ended March 31, 2001, as the warrants were for compensation unrelated to the December 8, 2000 private placement offering. The expense was determined based on the estimated fair value of the 100,000 issued and vested warrants. 41,200 of these warrants were exercised on August 11, 2003 and 58,800 warrants were exercised on August 21, 2003. On March 15, 2001, the Company entered into a one-year agreement with The Kriegsman Group ("Kriegsman") for assistance by Kriegsman with respect to financial consulting, planning, structuring, business strategy, public relations and promotions. This agreement was terminated by the Company, effective September 14, 2001. As compensation for these services, the Company paid a retainer fee to Kriegsman of $20,000 per month for the term of the agreement. The Company also granted Kriegsman warrants to purchase 250,000 shares of the Company's common stock at $10.75 per share. Warrants to purchase 100,000 shares vested immediately and the remaining 150,000 warrants did not vest and were cancelled. The warrants are exercisable over a five-year period and contain a cashless exercise provision. The Company recorded a general and administrative expense of approximately $422,000 during the year ended March 31, 2001 for the estimated fair value of the 100,000 issued and vested warrants. These 100,000 warrants were exercised on August 20, 2003. There were warrants outstanding as of March 31, 2001 to purchase 850,000 shares of the Company's common stock with an exercise price of $20.52 per share that were cancelled on April 20, 2001. -24- On January 31, 2002, the Company entered into a one year consulting agreement with Yorkshire Capital Limited ("Yorkshire") for services related to identifying investors and raising funds in connection with the February 2002 private placement offerings and assistance to be provided by Yorkshire to the Company with respect to financial consulting, planning, structuring, business strategy, public relations and promotions, among other items. In connection with the closing of the private placement offerings, the Company granted Yorkshire warrants to purchase 360,000 shares of the Company's common stock at prices ranging from $6.00 to $12.00 per share. Warrants to purchase 100,000 shares of the Company's common stock at an exercise price of $6.00 per share vested upon the closing of the private placement offerings. The remaining warrants did not vest and were cancelled. The warrants expire on February 14, 2007 and contain certain antidilution provisions. The Company may, upon 30 days' notice, redeem any vested warrants for $0.10 per share if the Company's Common Stock trades at 200% of the exercise price for 20 consecutive trading days. Yorkshire may exercise any vested warrants during such notice period. In addition, Yorkshire received 60,000 shares of the Company's common stock as additional consideration for identifying investors and raising funds in connection with the closing of the private placement offerings. As compensation for the consulting services, the Company was required to pay a retainer fee to Yorkshire of $10,000 per month for the term of the agreement. In February 2002, the Company, in connection with the Series A Convertible Preferred Stock private placement offering, issued warrants to purchase 400,250 shares of the Company's common stock at an exercise price of $6.00 per share of common stock. The warrants expire in February 2007. The warrant exercise period commences upon the conversion or the redemption of the Series A Convertible Preferred Stock that was concurrently issued to such warrant holder. At any time after the first anniversary of the date of grant and if the Company's common stock closes at $12.00 per share or above for 20 consecutive trading days, the Company may, upon 20 days' notice, redeem any unexercised portion of any warrants for a redemption fee of $.10 per share of common stock underlying the warrants. During the 20-day notice period, if the warrants are then exercisable as a result of the conversion or redemption of the Series A Convertible Preferred Stock, such warrant holder may then exercise all or a portion of the warrant by tendering the appropriate exercise price. The warrants contain certain antidilution provisions. The warrants issued in February 2002 to the holders of the Series A Convertible Preferred Stock were valued using the Black-Scholes option valuation model and the amount recorded of $908,535 was determined by applying the relative fair value method in relation to the estimated fair value of Series A Convertible Preferred Stock resulting in a $908,535 preferred deemed stock dividend calculated in accordance with the Emerging Issues Task Force ("EITF") Issue No. 00-27, "Application of Issue No. 98-5 to Certain Convertible Instruments." The deemed dividend on the Series A Convertible Preferred Stock was charged to deficit accumulated during the development stage immediately upon issuance, as the preferred stock is immediately convertible. The preferred stock deemed dividend of $908,535 was reported as a dividend in determining the net loss attributable to common stockholders in the accompanying statement of operations for the year ended March 31, 2002. -25- In addition, on February 1, 2002, the Company entered into an introductory brokerage agreement with Ace Champion, Ltd. ("Ace") and Pacific Dragon Group, Ltd. ("Pacific Dragon") (collectively, the "Introductory Brokers") for assistance to be provided by the Introductory Brokers to the Company with respect to obtaining funds in connection with the aforementioned February 2002 private placement offerings (see Note 3). As compensation for such services, Ace and Pacific Dragon received warrants to purchase 100,000 shares and 300,000 shares, respectively, of the Company's common stock at an exercise price of $6.00 per share, subject to certain conditions. The Company may, after February 22, 2003, upon 30 days' notice, provided that the Company's common stock has traded at or above 200% of the exercise price for 20 consecutive trading days, redeem any unexercised warrants for $0.10 per share, as defined. The Introductory Brokers may exercise their warrants during the 30-day notice period. The warrants expire on February 22, 2007 and contain certain antidilution provisions. In September 2002, in connection with of the Series B Convertible Preferred Stock private placement offering, the Company issued warrants to purchase 191,812 shares of the Company's common stock at an exercise price of $6.125 per share of common stock. The warrants expire at various dates in September 2007. The warrant exercise period commenced immediately upon issuance of the warrant. At any time after the first anniversary of the date of grant and if the Company's common stock closes above 200% of the exercise price for 20 consecutive trading days, the Company may, upon 20 days' notice, redeem any unexercised portion of any warrants for a redemption fee of $.10 per share of common stock underlying the warrants. During the 20-day notice period, if the warrants are then exercisable as a result of the conversion or redemption of the Series B Convertible Preferred Stock, such warrant holder may then exercise all or a portion of the warrants by tendering the appropriate exercise price. The warrants issued in September 2002 to the holders of the Series B Convertible Preferred Stock were valued using the Black-Scholes option valuation model and the amount recorded of $149,432 was determined by applying the relative fair value method in relation to the estimated fair value of Series B Convertible Preferred Stock resulting in a $149,432 preferred stock deemed dividend calculated in accordance with EITF Issue No. 00-27. The deemed dividend on the Series B Convertible Preferred Stock was charged to deficit accumulated during the development stage immediately upon issuance, as the preferred stock is immediately convertible. The preferred stock deemed dividend of $149,432 was reported as a dividend in determining the net loss attributable to common stockholders in the accompanying statement of operations for the year ended March 31, 2003. On July 16, 2003, the Company entered into an agreement with China Harvest International Ltd. ("China Harvest") for services to be provided to assist the Company in obtaining regulatory approval to conduct clinical trials in China. As consideration for these services, the Company granted China Harvest warrants to purchase 600,000 shares of common stock from the Company at $6.08 per share. These warrants are fully vested and have an exercise period of five years. During the year ended March 31, 2004, approximately $2,744,000 was recorded as general and administrative expenses, based on the estimated value of the warrants using the Black-Scholes option valuation model. -26- In January 2004, in connection with of the Series D Convertible Preferred Stock private placement offering, the Company issued warrants to purchase 200,000 shares of the Company's common stock at an exercise price of $16.00 per share of common stock. The warrants expire at various dates in January 2009. The warrant exercise period commenced immediately upon issuance of the warrant. At any time after the first anniversary of the date of grant and if the Company's common stock closes above 200% of the exercise price for 20 consecutive trading days, the Company may, upon 20 days' notice, redeem any unexercised portion of any warrants for a redemption fee of $.10 per share of common stock underlying the warrants. During the 20-day notice period, if the warrants are then exercisable as a result of the conversion or redemption of the Series D Convertible Preferred Stock, such warrant holder may then exercise all or a portion of the warrants by tendering the appropriate exercise price. The warrants issued in January 2004 to the holders of the Series D Convertible Preferred Stock were valued using the Black-Scholes option valuation model and the amount recorded of $1,973,287 was determined by applying the relative fair value method in relation to the estimated fair value of Series D Convertible Preferred Stock resulting in a $1,973,287 preferred stock deemed dividend calculated in accordance with EITF Issue No. 00-27. The deemed dividend on the Series D Convertible Preferred Stock was charged to deficit accumulated during the development stage immediately upon issuance, as the preferred stock is immediately convertible. The preferred stock deemed dividend of $1,973,287 was reported as a dividend in determining the net loss attributable to common stockholders in the accompanying statement of operations for the year ended March 31, 2004. The activity during the years ended March 31, 2002, 2003 and 2004 for the Company's warrants to purchase shares of common stock is summarized as follows: Weighted Number of Warrants Average Shares Price Range Exercise Price Outstanding as of March 31, 2001 2,275,000 $6.47-20.52 $ 12.85 Granted 1,160,250 6.00-12.00 7.01 Cancelled (1,000,000) 10.75-20.52 19.05 ------------ ------------ ------------ Outstanding as of March 31, 2002 2,435,250 6.00-16.00 7.52 Granted 250,977 6.00-15.00 6.64 Cancelled (260,000) 9.00-12.00 10.50 ------------ ------------ ------------ Outstanding as of March 31, 2003 2,426,227 6.00-16.00 7.11 Granted 1,120,833 6.00-16.00 9.16 Exercised (559,350) 6.00-16.00 8.00 ------------ ------------ ------------ Outstanding as of March 31, 2004 2,987,710 6.00-16.00 $ 7.70 ============ ============ ============ Exercisable as of March 31, 2002 1,775,000 $6.00-16.00 $ 7.43 Exercisable as of March 31, 2003 2,039,227 6.00-16.00 7.32 Exercisable as of March 31, 2004 2,977,712 6.00-16.00 7.72 -27- The following table summarizes information about outstanding warrants to purchase shares of the Company's common stock as of March 31, 2004: Exercise Price Warrants Per Share Outstanding Expiration Date $ 6.00 100,000 3/21/05 6.00 238,000 2/14/07 6.00 413,500 2/22/07 6.00 10,000 7/31/07 6.08 600,000 7/16/08 6.13 101,310 9/25/07 6.13 2,500 10/28/07 6.47 225,000 7/24/04 6.47 750,000 10/12/04 10.00 125,000 3/21/05 15.00 125,000 3/21/05 16.00 97,400 4/25/04 16.00 200,000 1/22/09 --------- Total warrants outstanding 2,987,710 ========= 8. COLLABORATIVE RESEARCH AND DEVELOPMENT ACTIVITIES The Company has various collaborative research agreements with commercial enterprises. Under the terms of these arrangements, the Company has agreed to perform best efforts research and development and, in exchange, the Company may receive advanced cash funding and may also earn additional fees for the attainment of certain milestones. The Company may receive royalties on the sales of such products that may result from these research and development activities and the other parties generally receive exclusive marketing and distribution rights for certain products for set time periods in specific geographic areas. The Company initially acquired its rights to the platform technology and dications developed by a consortium of universities consisting of The University of North Carolina at Chapel Hill ("UNC"), Georgia State University, Duke University and Auburn University (the "Scientific Consortium") pursuant to an agreement, dated January 15, 1997 (as amended, the "Consortium Agreement") among the Company, Pharm-Eco Laboratories, Inc. ("Pharm-Eco"), and UNC (to which each of the other members of the Scientific Consortium agreed shortly thereafter to become a party). The Consortium Agreement commits the parties to collectively research, develop, finance the research and development of, manufacture and market both the technology and compounds owned by the Scientific Consortium and previously licensed or optioned to Pharm-Eco and licensed to the Company in accordance with the Consortium Agreement (the "Current Compounds"), and all technology and compounds developed by the Scientific Consortium after January 15, 1997, through use of Company-sponsored research funding or National Cooperative Drug Development grant funding made available to the Scientific Consortium (the "Future Compounds" and, collectively with the Current Compounds, the "Compounds"). -28- The Consortium Agreement contemplated that upon the completion of the Company's initial public offering ("IPO") of shares of its common stock with gross proceeds of at least $10,000,000 by April 30, 1999, the Company and Pharm-Eco, with respect to the Current Compounds, and the Company and UNC, (on behalf of the Scientific Consortium), with respect to Future Compounds, would enter into license agreements for, or assignments of, the intellectual property rights relating to the Compounds held by Pharm-Eco and the Scientific Consortium; pursuant to which the Company would pay royalties and other payments based on revenues received for the sale of products based on the Compounds. The Company completed its IPO on April 26, 1999, with gross proceeds in excess of $10,000,000. Pursuant to the Consortium Agreement, both Pharm-Eco and the Scientific Consortium then became obligated to grant or assign to the Company an exclusive worldwide license to use, manufacture, have manufactured, promote, sell, distribute, or otherwise dispose of any products based directly or indirectly on all of the Current Compounds and Future Compounds. As a result of the closing of the IPO, the Company issued an aggregate of 611,250 shares of common stock, of which 162,500 shares were issued to the Scientific Consortium and 448,750 shares were issued to Pharm-Eco or persons designated by Pharm-Eco. Pursuant to the Consortium Agreement, the Company may, subject to the satisfaction of certain conditions, be required to issue 100,000 shares of common stock to the Scientific Consortium upon the filing by the Company of the first new drug application or an abbreviated new drug application with the Food and Drug Administration with respect to a product incorporating certain Compounds. In addition, the Company will pay the Scientific Consortium an aggregate royalty of up to 5.0% of net sales derived from the Compounds, except that the royalty rate payable on any Compound developed at Duke University will be determined by negotiations at the time such Compound is developed. In the event that the Company sublicenses its rights with respect to the Compounds to a third party, the Company will pay the Scientific Consortium a royalty based on a percentage of any royalties the Company receives, and a percentage of all signing, milestone and other payments made to the Company pursuant to the sublicense agreement. As contemplated by the Consortium Agreement, on January 28, 2002, the Company entered into a License Agreement with the Scientific Consortium whereby the Company received the exclusive license to commercialize dication technology and compounds developed or invented by one or more of the Consortium scientists after January 15, 1997, and which also incorporated into such License Agreement the Company's existing license with the Scientific Consortium with regard to the Current Compounds. In June 1999, the Company entered into a research and manufacturing agreement with Pharm-Eco for Pharm-Eco to produce good manufacturing practices quality, as defined, dicationic drugs and products for clinical testing and for early commercialization. Pharm-Eco was unable to manufacture certain required compounds and the Company subsequently engaged alternate suppliers who successfully manufactured the compounds. -29- In August 2000, Pharm-Eco and two of its senior executives filed suit in Delaware against the Company in connection with a dispute under the Consortium Agreement. The Company responded by denying the allegations and filing a counter-claim against Pharm-Eco for breach of contract. The Company filed a Motion for Summary Judgment, which was granted on February 21, 2001. In his Memorandum Opinion, the Vice Chancellor hearing the proceeding dismissed all of the plaintiffs' claims against the Company and held that Pharm-Eco had breached the Consortium Agreement by failing to grant or assign to the Company a license for the Current Compounds. On March 12, 2001, the Vice Chancellor signed a Final Order and Judgment directing Pharm-Eco to execute and deliver to the Company an agreement granting or assigning to the Company the license. On March 27, 2001, Pharm-Eco and the Company entered into an agreement assigning the license. No further claims against the Company remain in this proceeding, and on May 1, 2001, a Stipulation of Dismissal was filed with the Court. On April 20, 2001, the Company entered into a settlement agreement with Pharm-Eco and certain other parties resolving all remaining matters between them. Pursuant to this agreement, the Company received a cash payment of $1,000,000; an assignment from Pharm-Eco of various contract rights; and a termination of all of the Company's obligations to Pharm-Eco, including, without limitation, (a) the obligation to issue an aggregate of 850,000 warrants for shares of the Company's stock (see Note 7), (b) the obligation to issue shares of common stock upon the occurrence of a certain future event, (c) the obligation to pay a percentage of all non-royalty payments that the Company might receive under any sublicense that the Company might enter into with respect to certain compounds, and (d) certain accounts payable which Pharm-Eco claimed to be owed of approximately $159,000; and a release of any and all claims that Pharm-Eco may have had against the Company. The cash payment received and the accounts payable obligations which were forgiven, aggregating approximately $1,159,000, were recorded as a credit to (reduction of) research and development expense during the year ended March 31, 2002; as the Company had previously expensed the estimated fair value of the shares of common stock issued to Pharm-Eco at the time of the IPO and the accounts payable obligations, as research and development expense. The Company was required, under an agreement which has subsequently expired, to make quarterly research grants in the amount of $100,000 to UNC through April 30, 2002. During the years ended March 31, 2002 and 2003, the Company expensed grant payments to UNC of $400,000 and $100,000, respectively. Such payments were expensed as research and development costs. There were no grant payments to UNC during the year ended March 31, 2004. The Consortium Agreement provides that the Company is required to pay to UNC on behalf of the Scientific Consortium reimbursement of patent and patent-related fees, certain milestone payments and royalty payments based on revenue derived from the Scientific Consortium's dication technology. Each month on behalf of the inventor scientist or university, as the case may be, UNC submits an invoice to the Company for payment of patent-related fees related to current compounds or future compounds -30- incurred prior to the invoice date. The Company is also required to make milestone payments in the form of the issuance of 100,000 shares of its common stock to the Consortium when we file our initial New Drug Application ("NDA") or an Abbreviated New Drug Application ("ANDA") based on Consortium technology and are required to pay to UNC on behalf of the Scientific Consortium (other than Duke University) (i) royalty payments of up to 5% of our net worldwide sales of "current products" and "future products" (products based directly or indirectly on current compounds and future compounds, respectively) and (ii) a percentage of any fees we receive under sublicensing arrangements. With respect to products or licensing arrangements emanating from Duke University technology, the Company is required to negotiate in good faith with UNC (on behalf of Duke University) royalty, milestone or other fees at the time of such event, consistent with the terms of the Consortium Agreement. Under the License Agreement, the Company must also reimburse the cost of obtaining patents and assume liability for future costs to maintain and defend patents so long as the Company chooses to retain the license to such patents. In August 1999 and 2000, the Company was awarded three Small Business Innovation Research ("SBIR") grants aggregating approximately $1,429,000 from the National Institutes of Health ("NIH") to research various infections. During the year ended March 31, 2002, the Company recognized revenues of approximately $502,000, from these grants and expensed payments to UNC and certain other Scientific Consortium universities of approximately $163,000, for contracted research related to these grants. There is no additional funding available to the Company under these grants. In August 2001, the Company was awarded an additional SBIR grant from the NIH of approximately $144,000 as a three year grant to continue research on "Novel Procedures for Treatment of Opportunistic Infections." During the years ended March 31, 2002 and 2003, the Company recognized revenues of approximately $74,000 and $70,000 from this grant and expensed payments of approximately $65,000 and $70,000 to UNC and certain other Scientific Consortium universities for contracted research related to this grant. During the year ended March 31, 2004, no revenues or expenses were recorded related to this grant. During the years ended March 31, 2002, 2003 and 2004, the Company expensed approximately $438,000, $333,000 and $526,000, respectively, of other payments to UNC and certain other Scientific Consortium universities for patent related costs and other contracted research. Total payments expensed to UNC and certain other Scientific Consortium universities were approximately $1,066,000, $503,000 and $526,000 during the years ended March 31, 2002, 2003 and 2004, respectively. Included in accounts payable as of March 31, 2003 and 2004, was approximately $15,000 and $132,000, respectively, due to UNC and certain other Scientific Consortium universities. In November 2000, The Bill & Melinda Gates Foundation ("Gates Foundation") awarded a $15,114,000 grant to UNC to develop new drugs to treat Human Trypanosomiasis (African sleeping sickness) and Leishmaniasis. On March 29, 2001, UNC entered into a clinical research subcontract agreement with the Company, whereby the Company is to -31- receive up to $9,800,000, subject to certain terms and conditions, over a five year period to conduct certain clinical and research studies. In April 2003, the Gates Foundation awarded a $2,713,124 supplemental grant to UNC for the expansion of phase IIB/III clinical trials for treatment of Human Trypanosomiasis (African sleeping sickness) and improved manufacturing processes. The supplemental increase in the subcontract with UNC to the Company due to this amendment is $2,466,475, bringing the total available funding to the Company under this agreement to $12,266,475. The proceeds due to the Company under this arrangement are restricted to the development of new drugs for the treatment of Human Trypanosomiasis, Leishmaniasis, along with an improved manufacturing processes and must be segregated from other funds and used for specific purposes. During the years ended March 31, 2002, 2003 and 2004, the Company received installment payments under this grant of approximately $0, $3,380,000, and $1,025,000, respectively, and approximately $2,946,000, $1,389,000 and $2,114,000 was utilized for clinical and research purposes conducted and expensed during the years ended March 31, 2002, 2003 and 2004, respectively. The Company recognized revenues of approximately $2,946,000, $1,389,000 and $2,114,000 during the years ended March 31, 2002, 2003 and 2004, respectively, for services performed under the agreement. The remaining amount (approximately $2,554,000 and $1,465,000 as of March 31, 2003 and 2004, respectively) has been deferred and will be recognized as revenue over the term of the agreement as the services are performed. On May 4, 2001, the Company entered into a four-year subcontract agreement with a research company located in Switzerland for clinical research to be performed for the Company in connection with its subcontract agreement with UNC related to the Gates Foundation grants. The agreement provides for payments of up to approximately $1.2 million over the term of the agreement. The Company recognized expense of approximately $317,000, $498,000 and $425,000 during the years ended March 31, 2002, 2003 and 2004, respectively, related to this agreement. On April 22, 2002, the Company entered into a Confidentiality, Testing and Option Agreement with Neurochem, Inc. ("Neurochem"), a Canadian corporation, to supply Neurochem with selected dicationic compounds for the testing, evaluation and potential future licensing of such compounds for (i) the treatment and diagnosis of amyloidosis and the related underlying conditions of Alzheimer's Disease, cerebral amyloid angiopathy, primary amyloidosis, diabetes, rheumatic diseases and (ii) the treatments of conditions related to secondary amyloidosis. Under the agreement, Neurochem had the right to license technology related to the tested compounds upon the conclusion of the Confidentiality, Testing and Option Agreement, as defined in the agreement. On April 4, 2003, the Company notified Neurochem that the Confidentiality, Testing and Option Agreement had previously expired by its terms and that all rights granted to Neurochem thereunder had concurrently expired, including any right Neurochem may or may not have had to license such technology. -32- On November 26, 2003, the Company entered into a testing agreement with Medicines for Malaria Venture ("MMV"), a foundation established in Switzerland, and UNC. Pursuant to this agreement the Company, with the support of MMV and UNC, is to conduct a proof of concept study of the dicationic drug candidate DB289, including Phase II and Phase III human clinical trials, and will pursue drug development activities of DB289 alone, or in combination with other anti-malaria drugs, with the goal of obtaining marketing approval of a product for the treatment of malaria. Under the terms of the agreement, MMV has committed to advance funds to Immtech to pay for human clinical trials and regulatory preparation and filing costs for the approvals to market DB289 for treatment of malaria by at least one internationally accepted regulatory body and one malaria endemic country. The funding under this agreement is for the performance of specific research and is not subject to maximum funding amounts. The term of the funding portion of this agreement is three years and is subject to annual renewals. The Company has forecasted such costs to be approximately $8.2 million over the next three years. In return for this funding from MMV, Immtech is required to sell all malaria drugs derived from this research at a price not to exceed the cost to manufacture the drugs plus a reasonable profit (not to exceed 10% of the cost to manufacture) when selling into a malaria endemic country, as defined. Sales of malaria drugs to non-malaria endemic countries require that the Company pay a royalty not to exceed 7% of sales be paid to MMV until the amount funded under the agreement with UNC is refunded to MMV. MMV has agreed to fund the forecasted amount based on the progress achieved, including payment to the Company of approximately $668,000 during the year ended March 31, 2004 related to human clinical trials. The Company recognized revenues of approximately $302,000 during the year ended March 31, 2004 for expenses incurred related to activities within the scope of the agreement with MMV. At March 31, 2004, the Company has approximately $366,000 recorded as deferred revenue with respect to this agreement. 9. OTHER COMMITMENTS AND CONTINGENCIES Operating Leases - In December 1999, the Company entered into a lease of its main office and research facility under an operating lease that requires lease payments starting in March 2000 of approximately $12,100 per month through March 2003 and $12,800 from April 2003 through March 2005. The Company is required to pay certain real estate and occupancy costs. In July 1999, the Company began leasing an additional office facility from RADE, a related party, that is occupied by both the Company and RADE, on a month-to-month basis, for approximately $10,100 per month. Total rent expense was approximately $270,000, $285,000 and $310,000 for all leases during the years ended March 31, 2002, 2003, and 2004, respectively. As of March 31, 2004, future minimum lease payments required under the aforementioned noncancellable operating leases approximated the following: -33- Year Ending Lease March 31, Payments 2005 $ 153,000 --------- Total $ 153,000 ========= Other Contingencies - In connection with obtaining the consent of Criticare Systems, Inc. ("Criticare"), a significant stockholder of the Company, to the private placement of stock by NCHK in 1998, the Company transferred to Criticare, on July 2, 1998, certain of its intangible assets and 86,207 shares of the Company's common stock for $150,000. These intangible assets included (1) a license for rmCRP as a therapy for treating sepsis (a bacterial infection which quickly overwhelms the immune system and can lead to sudden death), and (2) rights to certain diagnostic products. The license granted to Criticare for rmCRP included patents and know-how developed by the Company. NextEra has licensed the rights for producing rmCRP back to the Company for use with sepsis applications. Criticare assigned the technology to another party and the assignee had until July 2, 1999, to raise a minimum of $500,000 to fund both the development of the sepsis technology and the initiation of clinical trials. The Company has not received notification from the assignee as to whether or not the funds have been raised. The Company is required to pay the cost of maintaining and defending the patents until the initial financing is completed by the assignee. The rights transferred to Criticare for the diagnostic products included rights to the Company's diagnostic products for measuring hemoglobin A1c in diabetic patients and Carbohydrate Deficient Transferrin ("CDT") as a marker in the blood for long-term alcohol abuse, as well as patents that have been issued for both technologies and exclusive worldwide rights from Northwestern University to develop and sell the products. Criticare is responsible for the maintenance and prosecution of the patents for both technologies. In June 2000, Technikrom, Inc. ("Technikrom") filed a claim against the Company with the American Arbitration Association in Chicago, Illinois. In that proceeding, Technikrom sought to recover $124,000 in fees, interest and costs for certain method development services provided to the Company relating to the purification of a protein known as rmCRP. The Company filed a counterclaim against Technikrom for fraudulent inducement of contract which sought compensatory damages of at least $224,000, plus interest and costs. The Company also sought a declaratory judgment that Technikrom, inter alia, failed to use its best efforts to develop a purification method within the time parameters set by the parties. The parties engaged an arbitrator and in November 2001 Technikrom was awarded a $95,000 settlement, which the Company subsequently paid. The Company is involved in various other claims and litigation incidental to its operations. In the opinion of management, ultimate resolution of these actions will not have a material effect on the Company's financial statements. -34- 10. OTHER RETIRED OBLIGATIONS Recapitalization - In connection with the Recapitalization (see Note 3) the following transactions occurred on July 24, 1998: o Criticare, a significant stockholder of the Company, who, prior to the Recapitalization, owned 1,000,000 shares of Series A Redeemable Preferred Stock, 1,200,000 shares of Series B Redeemable Preferred Stock and 198,708 shares of common stock, had advanced $597,722 to the Company. The advances were payable on demand. Criticare exchanged $597,722 of advances and $68,368 of related accrued interest for 145,353 shares of common stock. The Company also had certain notes payable to Criticare aggregating $148,777 and related accrued interest of $43,426 that were exchanged for 35,403 shares of common stock. The carrying value of the outstanding Criticare indebtedness in excess of the estimated fair value of the shares of common stock and cash exchanged was accounted for as additional paid-in capital. o Certain other stockholders exchanged $387,450 of advances for 196,824 shares of common stock. The Company recognized a gain on the extinguishment of debt of $80,404 for the outstanding indebtedness under the advances in excess of the estimated fair value of the 196,824 shares of common stock ($307,046). o Certain other notes payable aggregating $1,306,673, related accrued interest aggregating $337,290 and accounts payable aggregating $261,597 were exchanged for 227,398 shares of common stock and $203,450 cash. The Company recognized a gain on the extinguishment of debt of $1,347,361 for the outstanding aggregate indebtedness under such notes ($1,306,673), related accrued interest ($337,290) and accounts payable ($261,597) in excess of the estimated fair value of the shares of common stock ($354,749) and cash ($203,450) exchanged. o Series A and B Redeemable Preferred stockholders exchanged their preferred shares for an aggregate 1,195,017 shares of common stock. The holders of the Series A and Series B Redeemable Preferred Stock had cumulative dividend preferences at the rate of 8% per annum, compounded daily, of the liquidation value thereof, plus accumulated and unpaid dividends thereon, in preference to any dividend on common stock, payable when and if declared by the Company's Board of Directors. Dividends accrued whether or not they had been declared and whether or not there were profits, surplus or other funds of the Company legally available for the payment of dividends. The difference between the initial estimated fair value of the Series A Redeemable Preferred Stock and the aggregate redemption value of $440,119 was a premium which was amortized by a credit to retained earnings (deficit accumulated during the developmental stage) and a debit to the carrying value of the redeemable preferred stock during the period from issuance to the required redemption date, using the interest method. In addition, while the redeemable preferred shares were outstanding, dividends aggregating $1,783,354 were charged to retained earnings (deficit accumulated -35- during the development stage). The Series A and Series B Redeemable Preferred Stock had redemption (carrying) values of $2,780,324 and $2,797,260, respectively, as of the date of the Recapitalization. In connection with the Recapitalization, the Series A and Series B Redeemable Preferred stockholders agreed to accept 578,954 and 616,063 shares of common stock, respectively, for their shares of the preferred stock. The difference between the carrying value of the Series A and Series B Redeemable Preferred Stock and the estimated fair value of the common shares exchanged of $1,877,138 and $1,836,196, respectively, was credited to deficit accumulated during the development stage. Advances from Stockholder and Affiliate - As of March 31, 1999, the Company's president and NextEra had each advanced $25,000 to the Company. The advances were non-interest bearing and were repaid in May 1999. 11. SUPPLEMENTAL CASH FLOW INFORMATION The Company did not pay any income taxes or interest during the years ended March 31, 2002, 2003 and 2004. Non-Cash Investing and Financing Activities: During the years ended March 31, 2002, 2003 and 2004, the Company issued common stock, common stock options and warrants as compensation for services and engaged in certain other non-cash investing and financing activities. The amounts of these transactions are summarized as follows: -36- Years Ended March 31, ------------------------------------------- 2002 2003 2004 Expense related to issuance of common stock to nonemployees as compensation for services $ 982,390 $ 3,891,608 Expense related to issuance of common stock options as compensation for services $ 332,005 243,150 267,500 Expense related to issuance of warrants to purchase common stock as compensation for services 51,835 3,342,244 Issuance of common stock for offering costs 1,397,000 Convertible preferred stock dividends recorded 29,400 302,437 432,713 Issuance of common stock as payment of convertible preferred stock dividends 161,113 330,640 Issuance of common stock for conversions of convertible preferred stock 953,043 3,850,205 Exchange of ownership interests: Value of land use rights exchanged Land use rights (3,443,867) Minority interest 296,193 Value of leasehold improvement acquired 3,547,674 Issuance of common stock for acquisition of leasehold improvements: Fair value of land use rights acquired $ 3,501,522 Less: Minority interest (296,193) Cash paid for acquisition costs (204,924) Increase in accounts payable for acquisition costs (1,605) ----------- Issuance of common stock for acquisition of leasehold improvements $ 2,998,800 =========== * * * * * * -37-