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“体外”血脑屏障的特性:分子大小和亲脂性对脑血管内皮细胞药物转运速率的影响

Characterization of an "in vitro" blood-brain barrier: effects of molecular size and lipophilicity on cerebrovascular endothelial transport rates of drugs.

作者信息

van Bree J B, de Boer A G, Danhof M, Ginsel L A, Breimer D D

机构信息

Division of Pharmacology, State University of Leiden, The Netherlands.

出版信息

J Pharmacol Exp Ther. 1988 Dec;247(3):1233-9.

PMID:3204515
Abstract

The in vitro blood-brain barrier model described consisted of confluent monolayers of bovine cerebrovascular cells in primary cultures. Aim of the study was to investigate whether this type of model exhibits transport characteristics comparable to the in vivo blood-brain barrier and whether the cells in the cultured monolayers were able to form tight junctions, the most typical feature of the in vivo blood-brain barrier. Endothelial permeability of fluorescein-conjugated dextrans with increasing molecular size was correlated to monolayer pore shape, size and abundance by means of a mathematical model. Results showed that the in vitro pores had a longitudinal appearance with an effective pore size of 81 A and fractional pore area of 0.04%. These data indicate that the properties of the in vitro pores and in vivo tight junctions are comparable. The monolayer model was applied successfully to establish a relationship between endothelial permeability and drug lipophilicity, using several beta blocking agents and nonsteroidal anti-inflammatory drugs as model drugs. Results showed a sigmoidal relationship between these parameters, indicating the existence of a threshold lipophilicity for passive transendothelial transport.

摘要

所描述的体外血脑屏障模型由原代培养的牛脑血管细胞汇合单层组成。该研究的目的是调查这种类型的模型是否表现出与体内血脑屏障相当的转运特性,以及培养单层中的细胞是否能够形成紧密连接,这是体内血脑屏障最典型的特征。通过数学模型,将分子大小不断增加的荧光素偶联葡聚糖的内皮通透性与单层孔的形状、大小和丰度相关联。结果表明,体外孔呈纵向外观,有效孔径为81埃,孔隙面积分数为0.04%。这些数据表明,体外孔的特性与体内紧密连接相当。使用几种β受体阻滞剂和非甾体抗炎药作为模型药物,成功地应用单层模型建立了内皮通透性与药物亲脂性之间的关系。结果显示这些参数之间呈S形关系,表明存在被动跨内皮转运的亲脂性阈值。

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