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通过提取效率将简单乳腺模型中的一级摄取速率常数纳入血流限制的生理药代动力学模型。

Incorporation of first-order uptake rate constants from simple mammillary models into blood-flow limited physiological pharmacokinetic models via extraction efficiencies.

作者信息

Roth W L, Weber L W, Rozman K K

机构信息

Department of Pharmacology, Toxicology, and Therapeutics, University of Kansas Medical Center, Kansas City 66160, USA.

出版信息

Pharm Res. 1995 Feb;12(2):263-9. doi: 10.1023/a:1016239212118.

Abstract

Incorporation of First-Order Uptake Rate Constants from Simple Mammillary Models into Blood-Flow Limited Physiological Pharmacokinetic Models via Extraction Efficiencies. W. L. Roth, L. W. D. Weber, and K. Rozman (1995). Pharm. Res. 263-269. First-order rate constants obtained from classical pharmacokinetic models correspond to mammillary systems in which all of the blood (or plasma) is assumed to be located in a central compartment. In such models the rate at which chemicals are transported out of this pool and into another compartment is the product of the mass of chemical in the central compartment multiplied by a rate constant, which is not limited in magnitude by the blood flow, or the rate at which chemicals from the blood are delivered to the peripheral compartment. Most of the physiologically-based models published to date dispense with some of the information available from mammillary models by assuming that all of the chemical delivered by the flow of blood rapidly equilibrates and can be taken up by the tissue under the control of a "partition coefficient" (Rij = Cj/Ci). We show that the partition coefficient alone does not retain the uptake rate (kji) information available from a classical mammillary model, but that the uptake rate information can be incorporated via unitless extraction efficiency parameters, epsilon j.

摘要

通过提取效率将简单乳头模型中的一级摄取速率常数纳入血流限制的生理药代动力学模型。W. L. 罗斯、L. W. D. 韦伯和K. 罗兹曼(1995年)。《药物研究》263 - 269页。从经典药代动力学模型获得的一级速率常数对应于乳头系统,在该系统中,所有血液(或血浆)都假定位于中央室。在这类模型中,化学物质从该池转运到另一个室的速率是中央室中化学物质质量乘以一个速率常数的乘积,该速率常数在大小上不受血流限制,或者是血液中的化学物质输送到外周室的速率。迄今为止发表的大多数基于生理的模型通过假设血液流动输送的所有化学物质迅速达到平衡并可在“分配系数”(Rij = Cj/Ci)的控制下被组织摄取,从而舍弃了一些可从乳头模型获得的信息。我们表明,仅分配系数并不能保留经典乳头模型中可用的摄取速率(kji)信息,但摄取速率信息可通过无量纲提取效率参数εj纳入。

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