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血脑屏障生物学与方法学。

Blood-brain barrier biology and methodology.

作者信息

Pardridge W M

机构信息

Department of Medicine, UCLA School of Medicine, Los Angeles, California, CA 90095-1682, USA.

出版信息

J Neurovirol. 1999 Dec;5(6):556-69. doi: 10.3109/13550289909021285.

Abstract

The blood-brain barrier (BBB) is formed by epithelial-like high resistance tight junctions within the endothelium of capillaries perfusing the vertebrate brain. Because of the presence of the BBB, circulating molecules gain access to brain cells only via one of two processes: (i) lipid-mediated transport of small molecules through the BBB by free diffusion, or (ii) catalyzed transport. The latter includes carrier-mediated transport processes for low molecular weight nutrients and water soluble vitamins or receptor-mediated transport for circulating peptides (e.g., insulin), plasma proteins (e.g., transferrin), or viruses. While BBB permeability, per se, is controlled by the biochemical properties of the plasma membranes of the capillary endothelial cells, overall brain microvascular biology is a function of the paracrine interactions between the capillary endothelium and the other two major cells comprising the microcirculation of brain, i.e., the capillary pericyte, which shares the basement membrane with the endothelial cell, and the astrocyte foot process, which invests 99% of the abluminal surface of the capillary basement membrane in brain. Microvascular functions frequently ascribed to the capillary endothelium are actually executed by either the capillary pericyte or the capillary astrocyte foot process. With respect to BBB methodology, there are a variety of in vivo methods for studying biological transport across this important membrane. The classical physiologic techniques may now be correlated with modern biochemical and molecular biological approaches using freshly isolated animal or human brain capillaries. Isolated brain capillary endothelial cells can also be grown in tissue culture to form an 'in vitro BBB' model. However, BBB research cannot be performed using only the in vitro BBB model, but rather it is necessary to correlate observations made with the in vitro BBB model with in vivo studies.

摘要

血脑屏障(BBB)由灌注脊椎动物脑的毛细血管内皮内类似上皮细胞的高电阻紧密连接形成。由于血脑屏障的存在,循环分子仅通过以下两种过程之一进入脑细胞:(i)小分子通过自由扩散经脂质介导穿过血脑屏障的转运,或(ii)催化转运。后者包括低分子量营养物质和水溶性维生素的载体介导转运过程,或循环肽(如胰岛素)、血浆蛋白(如转铁蛋白)或病毒的受体介导转运。虽然血脑屏障的通透性本身由毛细血管内皮细胞质膜的生化特性控制,但整体脑微血管生物学是毛细血管内皮与构成脑微循环的其他两种主要细胞之间旁分泌相互作用的结果,即与内皮细胞共享基底膜的毛细血管周细胞,以及覆盖脑内毛细血管基底膜99%无腔表面的星形胶质细胞足突。通常归因于毛细血管内皮的微血管功能实际上是由毛细血管周细胞或毛细血管星形胶质细胞足突执行的。关于血脑屏障研究方法,有多种体内方法用于研究生物分子穿过这一重要膜的转运。经典的生理学技术现在可以与使用新鲜分离的动物或人脑毛细血管的现代生化和分子生物学方法相关联。分离的脑毛细血管内皮细胞也可以在组织培养中生长以形成“体外血脑屏障”模型。然而,血脑屏障研究不能仅使用体外血脑屏障模型进行,而是有必要将体外血脑屏障模型的观察结果与体内研究相关联。

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