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紧密连接骨架的分子结构和组装。

Molecular architecture and assembly of the tight junction backbone.

机构信息

Institute of Clinical Physiology/Nutritional Medicine, Medical Department, Division of Gastroenterology, Infectiology, Rheumatology, Charité - Universitätsmedizin Berlin, 12203 Berlin, Germany.

Leibniz-Institut für Molekulare Pharmakologie (FMP), 13125 Berlin, Germany.

出版信息

Biochim Biophys Acta Biomembr. 2020 Jul 1;1862(7):183279. doi: 10.1016/j.bbamem.2020.183279. Epub 2020 Mar 26.

Abstract

The functional and structural concept of tight junctions has developed after discovery of claudin and TAMP proteins. Many of these proteins contribute to epi- and endothelial barrier but some, in contrast, form paracellular channels. Claudins form the backbone of tight junction (TJ) strands whereas other proteins regulate TJ dynamics. The current joined double-row model of TJ strands and channels is crucially based on the linear alignment of claudin-15 in the crystal. Molecular dynamics simulations, protein docking, mutagenesis, cellular TJ reconstitution, and electron microscopy studies largely support stability and functionality of the model. Here, we summarize in silico and in vitro data about TJ strand assembly including comparison of claudin crystal structures and alternative models. Sequence comparisons, experimental and structural data substantiate differentiation of classic and non-classic claudins differing in motifs related to strand assembly. Classic claudins seem to share a similar mechanism of strand formation. Interface variations likely contribute to TJ strand flexibility. Combined in vitro/in silico studies are expected to elucidate mechanistic keys determining TJ regulation.

摘要

紧密连接的功能和结构概念是在发现 Claudin 和 TAMP 蛋白后发展起来的。这些蛋白质中的许多都有助于上皮和内皮屏障的形成,但也有一些形成细胞旁通道。Claudin 构成紧密连接 (TJ) 链的骨干,而其他蛋白质则调节 TJ 的动态。目前 TJ 链和通道的联合双排模型主要基于 Claudin-15 在晶体中的线性排列。分子动力学模拟、蛋白质对接、诱变、细胞 TJ 重建和电子显微镜研究在很大程度上支持了该模型的稳定性和功能性。在这里,我们总结了关于 TJ 链组装的计算和体外数据,包括 Claudin 晶体结构和替代模型的比较。序列比较、实验和结构数据证实了经典和非经典 Claudin 的分化,它们在与链组装相关的基序上有所不同。经典 Claudin 似乎共享类似的链形成机制。界面变化可能有助于 TJ 链的灵活性。预计结合体外/计算研究将阐明决定 TJ 调节的机制关键。

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