A preliminary pharmacokinetic study of the antimalarial drugs, proguanil and chlorproguanil

Author:

Watkins W M123,Chulay J D4,Sixsmith D G1,Spencer H C15,Howells R E3

Affiliation:

1. Biomedical Sciences Research Centre, Kenya Medical Research Institute, Nairobi

2. Wellcome Trust Research Laboratories, PO Box 43640 Nairobi, Kenya

3. Liverpool School of Tropical Medicine

4. Department of Immunology, Walter Reed Army Institute of Research, Washington DC

5. Division of Parasitic Diseases, Centers for Disease Control, Atlanta, GA 30333, USA

Abstract

Abstract Pharmacokinetic parameters for cycloguanil and chlorcycloguanil, the active metabolites of proguanil (Paludrine] and chlorproguanil (Lapudrine) have been measured in a bioassay which assesses the in-vitro growth inhibition of a cycloguanil- and chlorcycloguanil-sensitive strain of Plasmodium falciparum produced by dilutions of plasma collected after oral administration of the pro-drugs. A single compartment model is applicable for cycloguanil with mean rate constants of elimination of 0.0624 h−1 and availability of 0.2398 h−1. The elimination profile for chlorcycloguanil indicates partition of drug into more than one compartment. In 2 of 10 subjects dosed with proguanil and 1 of 11 subjects dosed with chlorproguanil, the active metabolite levels were significantly lower than the mean for the other subjects. Abnormally low cycloguanil or chlorcycloguanil plasma levels may be of importance in relation to effective prophylaxis against malaria.

Publisher

Oxford University Press (OUP)

Subject

Pharmaceutical Science,Pharmacology

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