Clotrimazole (Bay b 5097): In Vitro and Clinical Pharmacological Studies

Burgess, Michael A.; Bodey, Gerald P.

doi:10.1128/aac.2.6.423

Cited by 63 publications

(25 citation statements)

References 21 publications

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“…Pharmacokinetic information on CLT in humans indicates that, in healthy subjects after a single oral dose of 1 g CLT (Ϸ15 mg͞kg body weight), plasma levels reach mean peak concentrations of about 2 M within 2-4 hr of administration (15,16). Similar and even higher CLT levels have been found by others after oral administration of comparable doses (12,17). Most of CLT in plasma is bound to lipoproteins, 4% is bound to albumin, and less than 1% appears to be free (15).…”

Section: Discussionsupporting

confidence: 58%

Potent antimalarial activity of clotrimazole in in vitro cultures of Plasmodium falciparum

Tiffert

Ginsburg

Krugliak

et al. 2000

Proc. Natl. Acad. Sci. U.S.A.

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The increasing resistance of the malaria parasite Plasmodium falciparum to currently available drugs demands a continuous effort to develop new antimalarial agents. In this quest, the identification of antimalarial effects of drugs already in use for other therapies represents an attractive approach with potentially rapid clinical application. We have found that the extensively used antimycotic drug clotrimazole (CLT) effectively and rapidly inhibited parasite growth in five different strains of P. falciparum, in vitro, irrespective of their chloroquine sensitivity. The concentrations for 50% inhibition (IC50), assessed by parasite incorporation of [ 3 H]hypoxanthine, were between 0.2 and 1.1 M. CLT concentrations of 2 M and above caused a sharp decline in parasitemia, complete inhibition of parasite replication, and destruction of parasites and host cells within a single intraerythrocytic asexual cycle (Ϸ48 hr). These concentrations are within the plasma levels known to be attained in humans after oral administration of the drug. The effects were associated with distinct morphological changes. Transient exposure of ring-stage parasites to 2.5 M CLT for a period of 12 hr caused a delay in development in a fraction of parasites that reverted to normal after drug removal; 24-hr exposure to the same concentration caused total destruction of parasites and parasitized cells. Chloroquine antagonized the effects of CLT whereas mefloquine was synergistic. The present study suggests that CLT holds much promise as an antimalarial agent and that it is suitable for a clinical study in P. falciparum malaria. In the course of an investigation on the homeostasis of human red cells infected in vitro with the human malaria parasite Plasmodium falciparum, we found that clotrimazole (CLT), an imidazole derivative used as an antifungal agent (1), had a powerful growth-inhibiting effect on the parasite. The vast clinical experience, proven tolerance, and unique lack of acquired fungal resistance to CLT prompted a detailed investigation of its antimalarial effects in cultures of P. falciparum to assess its clinical potential. In this study, we report the in vitro effects of CLT on P. falciparum cultures by assessing the timeand concentration-dependent changes in parasite growth, parasite morphology, stage-specific development, and parasite replication. Materials and MethodsCultures. Five different laboratory strains of P. falciparum [A4 (2), W2, NF54, HB3, and FCR] were cultured in human erythrocytes by standard methods (3) under a low oxygen atmosphere. The culture medium was RPMI 1640, supplemented with 40 mM Hepes, 25 mg͞liter gentamicin sulfate, 10 mM D-glucose, 2 mM glutamine, and either 8.5% (vol͞vol) pooled human serum (A4 clone), or 10% heat-inactivated plasma (strains W2, NF54, HB3, and FCR). Culture media, with or without CLT, were changed daily, unless otherwise indicated. Parasites were synchronized at the ring stage with D-sorbitol (4) for all experiments. Initial parasitemias varied between 2% and 7% for the different e...

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Section: Discussionsupporting

confidence: 58%

Potent antimalarial activity of clotrimazole in in vitro cultures of Plasmodium falciparum

Tiffert

Ginsburg

Krugliak

et al. 2000

Proc. Natl. Acad. Sci. U.S.A.

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“…Pharmacokinetic studies in humans demonstrated a progressive decline over several days in the serum concentrations of clotrimazole after oral administration; these data supported the hypothesis of liver enzyme induction by the drug (43,141). Unacceptable side effects include high incidences of gastrointestinal disturbances following oral administration of clotrimazole (43,47,339) and alterations in hepatic and adrenal functions (300 (181).…”

Section: Clotrimazolesupporting

confidence: 58%

“…Clotrimazole is more active than griseofulvin and nystatin against dermatophytes as well. Its broad spectrum and potent activity have been confirmed in many studies (26,43,220,264,345). Very short contact time is required for clotrimazole to effect its antifungal activity (246), and as with the other imidazoles, the suggested mode of action appears to be disturbance of the fungal cell membrane.…”

Section: Clotrimazolementioning

confidence: 79%

Overview of medically important antifungal azole derivatives

1988

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Fungal infections are a major burden to the health and welfare of modern humans. They range from simply cosmetic, non-life-threatening skin infections to severe, systemic infections that may lead to significant debilitation or death. The selection of chemotherapeutic agents useful for the treatment of fungal infections is small. In this overview, a major chemical group with antifungal activity, the azole derivatives, is examined. Included are historical and state of the art information on the in vitro activity, experimental in vivo activity, mode of action, pharmacokinetics, clinical studies, and uses and adverse reactions of imidazoles currently marketed (clotrimazole, miconazole, econazole, ketoconazole, bifonazole, butoconazole, croconazole, fenticonazole, isoconazole, oxiconazole, sulconazole, and tioconazole) and under development (aliconazole and omoconazole), as well as triazoles currently marketed (terconazole) and under development (fluconazole, itraconazole, vibunazole, alteconazole, and ICI 195,739).

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“…We found in the spectrophotometric assay of IC1/2 that all of the drugs were active, even compared with concentrations achieved in serum after systemic administration (4,5,7,11,12,14,19). Their activity was very similar, with clotrimazole slightly less active.…”

Section: Discussionmentioning

confidence: 99%

Inhibition and killing of Candida albicans in vitro by five imidazoles in clinical use

Lefler¹,

Da²

1984

Antimicrob Agents Chemother

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Five imidazoles (clotrimazole, econazole, ketoconazole, miconazole, and tioconazole) in clinical use were compared for their ability to inhibit and kill Candida albicans. Eleven isolates were obtained from patients before therapy. By spectrophotometric determination of 5%o growth inhibition, all isolates were inhibited at low concentrations, with clotrimazole slightly less active than the other four drugs. By the conventional MIC determination, tioconazole was more active than all of the others (P < 0.01) except clotrimazole. In killing (minimum fungicidal concentration [MFC] assay), tioconazole was the most active by several analyses. Studies of the kinetics of killing indicated that the drugs studied could kill under conditions used for the MFC determination and that tioconazole and ketoconazole could kill particularly rapidly. If the drug was washed from the cells before subculturing, concentrations above the MFC were required to kill, but tioconazole could produce a lethal lesion in all cells virtually instantaneously. These findings are pertinent to MFC and killing kinetics methodology and to the observation of drug persistence after topical application. The results differ from some previous in vitro comparisons made with different methods. They are relevant to conclusions about drug mechanisms based on their abilities to inhibit and to kill, and they underscore the need to study various assay methods and fungal species.

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Clotrimazole (Bay b 5097): In Vitro and Clinical Pharmacological Studies

Cited by 63 publications

References 21 publications

Potent antimalarial activity of clotrimazole in in vitro cultures of Plasmodium falciparum

Potent antimalarial activity of clotrimazole in in vitro cultures of Plasmodium falciparum

Overview of medically important antifungal azole derivatives

Inhibition and killing of Candida albicans in vitro by five imidazoles in clinical use

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