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人用亲脂性阿莫西林前体药物沙莫西林的药代动力学和处置情况。

Human pharmacokinetics and disposition of sarmoxicillin, a lipophilic amoxicillin prodrug.

作者信息

Smyth R D, Pfeffer M, Van Harken D R, Cohen A, Hottendorf G H

出版信息

Antimicrob Agents Chemother. 1981 Jun;19(6):1004-12. doi: 10.1128/AAC.19.6.1004.

Abstract

Sarmoxicillin, an amoxicillin prodrug, is the methoxymethyl ester of hetamoxicillin. Esterification converted amoxicillin from an amphoteric to a cationic compound and resulted in a 30- to 600-fold increase in lipid partitioning. Oral absorption studies in normal subjects demonstrated that sarmoxicillin was only partially hydrolyzed by nonenzymatic and gut or hepatic first-pass metabolism and that significant quantities of intact ester appeared in the systemic circulation. Sarmoxicillin was converted to amoxicillin in plasma by hydrolysis of the acetone penicinate and the methoxymethyl ester bonds. Significant amoxicillin levels were demonstrated in saliva after administration of sarmoxicillin, but not amoxicillin, over a 250- to 1,000-mg dose range. Differences in the absorption, distribution, or metabolism of amoxicillin were also evident in the lower plasma amoxicillin maximum concentration and area under the curve and longer half-life after sarmoxicillin administration. Differences in the distribution of this lipophilic ester could result in a significant increase in tissue penetration and subsequent therapeutic efficacy of amoxicillin when administered as sarmoxicillin.

摘要

沙莫西林是阿莫西林的前体药物,是海他西林的甲氧基甲酯。酯化作用将阿莫西林从两性化合物转变为阳离子化合物,导致脂质分配增加30至600倍。在正常受试者中进行的口服吸收研究表明,沙莫西林仅通过非酶促以及肠道或肝脏首过代谢被部分水解,并且大量完整的酯出现在体循环中。沙莫西林通过丙酮青霉素酯键和甲氧基甲酯键的水解在血浆中转化为阿莫西林。在250至1000毫克剂量范围内给药后,沙莫西林给药后唾液中出现显著的阿莫西林水平,但阿莫西林给药后则未出现。在沙莫西林给药后,血浆阿莫西林的最大浓度、曲线下面积较低以及半衰期较长,这也表明阿莫西林在吸收、分布或代谢方面存在差异。当以沙莫西林形式给药时,这种亲脂性酯的分布差异可能会导致阿莫西林的组织穿透力显著增加以及随后的治疗效果显著提高。

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