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[内皮细胞屏障功能障碍中的微管系统:外周微管的解聚及胞质内微管的重组]

[The microtubule system in endothelial barrier dysfunction: disassembly of peripheral microtubules and microtubules reorganization in internal cytoplasm].

作者信息

Smurova K M, Biriukova A A, Verin A D, Alieva I B

出版信息

Tsitologiia. 2008;50(1):49-55.

Abstract

Endothelial cell barrier dysfunction is often associated with dramatic cytoskeletal reorganization, activation of actomyosin contraction and finally gap formation. At present time the role of microtubules in endothelial cell barrier regulation is not fully understood, however a number of observations allow to assume that microtubules reaction is the extremely important part in development of endothelial dysfunction. These observations have been forced us to examine the role of microtubule system reorganization in endothelial cell barrier regulation. In quiescent endothelial cells microtubule density is the highest in the centrosome region and insignificant near the cell margin. The analysis of microtubules distribution after specific antibodies staining using the method of measurement of their fluorescence intensity has shown that in control endothelial cells the reduction of fluorescence intensity from the cell center to its periphery is described by the equation of an exponential regression. The hormone agent, thrombin (25 nM), causes rapid increase of endothelial cell barrier permeability accompanied by fast decrease in quantity of peripheral microtubules and reorganization of microtubule system in internal cytoplasm of endothelial cells (the decrease of fluorescence intensity is described by the equation of linear regress already through 10 min after the beginning of the treatment). Both effects are reversible -- through 60 min after the beginning of the treatment the microtubule network does not differ from normal one, so the microtubule system is capable to adapt for influence of a natural regulator thrombin. The microtubules reaction develops more quickly, than reorganization of the actin filaments system, which responsible for the subsequent changes in the cell shape during barrier dysfunction. Apparently, the microtubules are the first part in a circuit of the reactions leading to the pulmonary endothelial cell barrier compromise.

摘要

内皮细胞屏障功能障碍通常与显著的细胞骨架重组、肌动球蛋白收缩激活以及最终的间隙形成有关。目前,微管在内皮细胞屏障调节中的作用尚未完全明确,然而,一些观察结果使我们推测微管反应是内皮功能障碍发展过程中极其重要的部分。这些观察结果促使我们研究微管系统重组在内皮细胞屏障调节中的作用。在静止的内皮细胞中,微管密度在中心体区域最高,而在细胞边缘附近则不显著。使用荧光强度测量方法对特异性抗体染色后的微管分布进行分析表明,在对照内皮细胞中,从细胞中心到其周边的荧光强度降低符合指数回归方程。激素因子凝血酶(25 nM)会导致内皮细胞屏障通透性迅速增加,同时外周微管数量快速减少,内皮细胞内细胞质中的微管系统发生重组(处理开始后10分钟,荧光强度的降低就符合线性回归方程)。这两种效应都是可逆的——处理开始后60分钟,微管网络与正常网络无异,因此微管系统能够适应天然调节因子凝血酶的影响。微管反应比肌动蛋白丝系统的重组发展得更快,而肌动蛋白丝系统在屏障功能障碍期间负责细胞形状的后续变化。显然,微管是导致肺内皮细胞屏障受损的反应过程中的首要部分。

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