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药物药代动力学与二氧化碳呼气试验

Drug pharmacokinetics and the carbon dioxide breath test.

作者信息

Lane E A, Parashos I

出版信息

J Pharmacokinet Biopharm. 1986 Feb;14(1):29-49. doi: 10.1007/BF01059282.

Abstract

The interrelationship of the pharmacokinetics of a drug and the expiration of carbon dioxide formed as a metabolite have been studied. The pharmacokinetic characteristics of the drug that affect the usefulness of the carbon dioxide excretion as a measure of liver function were examined by means of computer simulations. The parent drug extraction ratio, fraction demethylated, volume of distribution, and absorption rate of an oral dosage form all contribute to the carbon dioxide breath test result. A drug that would be a useful substrate when the carbon dioxide breath test is used as a probe for changes in liver function should be at least 50% metabolized by demethylation, have a hepatic extraction ratio of 0.2-0.5, and be administered in a form that is rapidly absorbed.

摘要

药物的药代动力学与作为代谢产物形成的二氧化碳呼出之间的相互关系已得到研究。通过计算机模拟研究了影响二氧化碳排泄作为肝功能指标有效性的药物药代动力学特征。母体药物提取率、去甲基化分数、分布容积和口服剂型的吸收率均对二氧化碳呼气试验结果有影响。当二氧化碳呼气试验用作肝功能变化的检测指标时,一种有用的底物药物应至少50%通过去甲基化代谢,肝提取率为0.2 - 0.5,并以快速吸收的剂型给药。

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