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犬静脉注射后异烟肼的血浆和淋巴动力学

Isoniazid plasma and lymph kinetics after intravenous injection in dogs.

作者信息

Blanc M, Steimer J L, Boyer C, Plusquellec Y, Cotonat J

出版信息

Arzneimittelforschung. 1984;34(10):1283-8.

PMID:6542789
Abstract

Isoniazid pharmacokinetics after bolus intravenous injection in dogs has been studied using concentration measurements in plasma and in the lymph collected as the outflow of the thoracic duct. Simple graphical analysis as well as fitting of the data indicates that the plasma concentration exhibits biexponential decrease whereas three exponential components are detected in lymphatic kinetics. The discrepancy in the number of exponentials cannot be accounted for by a catenary three-compartment model. Another model, which is compatible with the anatomo-physiological characteristics of the lymphatic circulation is proposed. To account for transfer delays between the plasma-lymph exchange areas and the site of measurement, we assume that the drug concentration in the lymph collected at the extremity of the thoracic duct is the convolution of the interstitial lymphatic concentration with an exponential distribution of transit times. Assuming, furthermore, that a rapid equilibrium between plasma and interstitial lymph is established and that variations in the lymphatic flow are negligible, this model provides an adequate description of isoniazid plasma and lymph kinetics as can be judged from: 1. the satisfactory adjustment of model predicted values to the concentration measurements after global nonlinear least-squares fitting of plasmatic and lymphatic data; 2. the agreement of the estimated isoniazid pharmacokinetic parameters with values reported in literature. This agreement suggests that lymphatic concentrations at the exit of the thoracic duct give an indirect and distorted picture of interstitial fluid isoniazid levels whose kinetics, in fact, closely follows that existing in plasma.

摘要

通过测量犬大剂量静脉注射异烟肼后血浆和胸导管流出的淋巴液中的浓度,对其药代动力学进行了研究。简单的图形分析以及数据拟合表明,血浆浓度呈双指数下降,而淋巴动力学中检测到三个指数成分。指数数量的差异不能用链状三室模型来解释。提出了另一个与淋巴循环的解剖生理特征相符的模型。为了解释血浆 - 淋巴交换区域与测量部位之间的转运延迟,我们假设在胸导管末端收集的淋巴液中的药物浓度是间质淋巴浓度与转运时间的指数分布的卷积。此外,假设血浆与间质淋巴之间迅速达到平衡,并且淋巴液流量的变化可忽略不计,该模型能够充分描述异烟肼的血浆和淋巴动力学,这可以从以下方面判断:1. 在对血浆和淋巴数据进行全局非线性最小二乘拟合后,模型预测值与浓度测量值的满意调整;2. 估计的异烟肼药代动力学参数与文献报道值的一致性。这种一致性表明,胸导管出口处的淋巴浓度间接且扭曲地反映了间质液中异烟肼的水平,实际上其动力学与血浆中的情况密切相关。

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