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抗疟药物氯胍和氯丙胍的初步药代动力学研究。

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

作者信息

Watkins W M, Chulay J D, Sixsmith D G, Spencer H C, Howells R E

出版信息

J Pharm Pharmacol. 1987 Apr;39(4):261-5. doi: 10.1111/j.2042-7158.1987.tb06263.x.

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.

摘要

在一项生物测定中,已对环氯胍和氯环氯胍(分别是氯胍(百乐君)和氯丙胍(拉布君)的活性代谢产物)的药代动力学参数进行了测定。该生物测定评估了口服前体药物后采集的血浆稀释液对环氯胍和氯环氯胍敏感的恶性疟原虫菌株的体外生长抑制作用。单室模型适用于环氯胍,其平均消除速率常数为0.0624 h⁻¹,可利用度为0.2398 h⁻¹。氯环氯胍的消除曲线表明药物分布于多个房室。在服用氯胍的10名受试者中有2名,以及服用氯丙胍的11名受试者中有1名,其活性代谢产物水平显著低于其他受试者的平均值。环氯胍或氯环氯胍血浆水平异常低可能对疟疾的有效预防具有重要意义。

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