Water-soluble lipopeptide L-693,989 was evaluated for its antipneumocystis activity in rats. Rats from colonies with latent Pneumocystis carinii infections were immunosuppressed with dexamethasone for 6 weeks to facilitate the development of acute P. carinii pneumonia (PCP). After 6 weeks, the rats were maintained on dexamethasone and were treated twice daily for 4 days with various concentrations of L-693,989. At a dose of 0.15 mg/kg of body weight, the compound effectively eliminated 90%o of the cysts in 4 days. Trophozoite forms of P. carinii were still present in these animals, as determined by using a P. carinii-specific DNA probe. A 3-week therapy study showed that the trophozoite load did not expand during treatment and that the trophozoites already present at the initiation of therapy appeared to persist. This may be a consequence of the stage specificity of the compound for cyst development and the severe immunosuppressive effects of dexamethasone on rats. When evaluated as a daily parenteral prophylactic agent, L-693,989 was effective in preventing the development of both P. carinii cysts and trophozoites, demonstrating its potential for use in prophylaxis and implying that the cyst stage ofP. carinii is an obligatory step in trophozoite multiplication. The foamy exudate commonly associated with P. carinii infections was absent in the lungs of rats on prophylaxis. The compound was also evaluated via oral administration and was found to have a 90%Yo effective dose of 32 mg/kg for therapy of acute infections and 5 mg/kg for daily prophylaxis.Pneumocystis carinii pneumonia (PCP) is a life-threatening disease which occurs in immunocompromised patients, especially those afflicted with AIDS. Although agents are available for the treatment and prevention of PCP, there is an unusually high incidence of adverse reactions to these treatments, particularly in patients with AIDS (14). Consequently, safer agents for controlling this disease are needed. We recently reported a novel method for controlling P.cainni infections in rodents using 1,3-p-glucan synthesis inhibitors (12). The more potent of these inhibitors, the lipopeptide natural product L-671,329 (Fig. 1), rapidly eliminates P. carinii cysts in 4 days when it is used to treat immunosuppressed rats with acute PCP. In addition to the antipneumocystis activity, L-671,329 is also effective against Candida infections in animal models (2). The lack of a counterpart for 1,3-p-glucan synthesis in humans should allow for selective killing of P. carinii and Candida spp. A shortcoming of L-671,329 and similar lipopeptides is their insolubility in aqueous solution, limiting their potential use as intravenous agents. Although cosolvent systems have been used for some insoluble drugs in the past, many of these formulations may no longer be acceptable because of adverse reactions (4, 8, 10); thus, water-soluble compounds are much more desirable. Therefore, a semisynthetic watersoluble prodrug, L-693,989 (Fig. 1 To determine the potential clinical use of L-693,989 in tre...
