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单次口服给药后,使用游离血浆水杨酸浓度和代谢物尿排泄率的水杨酸药代动力学模型表示。

Model representation of salicylate pharmacokinetics using unbound plasma salicylate concentrations and metabolite urinary excretion rates following a single oral dose.

作者信息

Shen J, Wanwimolruk S, Purves R D, McQueen E G, Roberts M S

机构信息

Department of Pharmacy, University of Otago Medical School, Dunedin, New Zealand.

出版信息

J Pharmacokinet Biopharm. 1991 Oct;19(5):575-95. doi: 10.1007/BF01062964.

Abstract

The pharmacokinetics of salicylic acid (SA) and its metabolites have been studied in 5 volunteers after administration of 3 g salicylic acid (as sodium salicylate) and collection of serial samples of blood and urine. SA and its metabolites were assayed with a HPLC method specific for each species. The urinary excretion rates of individual metabolites were analyzed using unbound plasma SA concentrations and Lineweaver-Burke plots. The analysis confirmed that the formation of SA urate (SU) and SA phenolic glucuronide (SPG) metabolites are saturable processes, and showed that the Michaelis-Menten values derived are consistent with earlier estimates derived solely from urinary data. The unbound salicylate plasma concentration-time profiles were then analyzed with various models assuming either saturable clearances for metabolite formation and/or saturable protein binding. The data were best described with a model that included both saturable protein binding and saturable metabolism. The model assumed first-order absorption kinetics and instantaneous distribution into extravascular and tissue compartments. The model was validated by comparing predicted relationships between the apparent volume of distribution, clearance, and plasma salicylate concentrations with previous relationships obtained using steady state data.

摘要

在5名志愿者服用3克水杨酸(以水杨酸钠形式)并采集系列血液和尿液样本后,对水杨酸(SA)及其代谢产物的药代动力学进行了研究。SA及其代谢产物采用针对每种物质的高效液相色谱法进行测定。使用游离血浆SA浓度和Lineweaver-Burke图分析了各个代谢产物的尿排泄率。分析证实,SA尿酸盐(SU)和SA酚醛葡萄糖醛酸苷(SPG)代谢产物的形成是可饱和过程,并表明推导得到的米氏常数与仅从尿液数据得出的早期估计值一致。然后,假设代谢产物形成的清除率和/或蛋白质结合是可饱和的,用各种模型分析游离水杨酸血浆浓度-时间曲线。用一个既包括可饱和蛋白质结合又包括可饱和代谢的模型能最好地描述这些数据。该模型假定为一级吸收动力学,并瞬间分布到血管外和组织隔室。通过将分布表观体积、清除率和血浆水杨酸浓度之间的预测关系与先前使用稳态数据获得的关系进行比较,对该模型进行了验证。

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