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放线菌素-D在比格犬体内分布动力学模型。

A model for the kinetics of distribution of actinomycin-D in the beagle dog.

作者信息

Lutz R J, Galbraith W M, Dedrick R L, Shrager R, Mellett L B

出版信息

J Pharmacol Exp Ther. 1977 Mar;200(3):469-78.

PMID:557542
Abstract

A pharmacokinetic model is presented for the distribution of actinomycin-D in the beagle dog. A simple, flow-limited model provides good simulations of the data at doses of 0.6 mg/m2 (0.03 mg/kg) and 2.7 mg/m2 (0.135 mg/kg) for most normal tissues. This implies that uptake of actinomycin-D in vivo is limited by tissue blood flow rate rather than by cell permeability. However, uptake by the testes is restricted by a blood-testis barrier, and a linear membrane-limited model is required to simulate the testis data. Linear binding of actinomycin-D to tissue is suggested by the fact that tissue concentrations are proportional to dose at least up to the lethal dose in dogs. The binding is also rapid and reversible as indicated by the tissue concentration curves which are parallel to the time course of the declining plasma curves.

摘要

本文提出了一个关于放线菌素-D在比格犬体内分布的药代动力学模型。一个简单的血流限制模型能够很好地模拟大多数正常组织在剂量为0.6 mg/m²(0.03 mg/kg)和2.7 mg/m²(0.135 mg/kg)时的数据。这意味着放线菌素-D在体内的摄取受组织血流速率限制,而非细胞通透性限制。然而,睾丸的摄取受到血睾屏障的限制,因此需要一个线性膜限制模型来模拟睾丸的数据。放线菌素-D与组织的线性结合可由以下事实表明:至少在犬的致死剂量之前,组织浓度与剂量成正比。组织浓度曲线与血浆下降曲线的时间进程平行,这表明结合也是快速且可逆的。

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