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首页> 外文期刊>Molecular simulation >Intrinsically disordered regions mediate macromolecular assembly of the Slit diaphragm proteins associated with Nephrotic syndrome
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Intrinsically disordered regions mediate macromolecular assembly of the Slit diaphragm proteins associated with Nephrotic syndrome

机译:本质无序区域介导与肾病综合征相关的狭缝膜片蛋白的大分子组装

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摘要

The glomerular filtration barrier (GFB) of the kidney plays an instrumental role in preventing the excretion of large molecules and ensuring the formation of ultra-filtrated urine. Podocytes are essential components of GFB that provide epithelial coverage to the fine glomerular capillaries. Slit-diaphragm (SD) that forms the sole contact between adjacent foot-processes of the podocytes consists of multimeric protein assemblies. SD serves as a molecular sieve and confers size and charge-selective barrier. Nephrin, podocin, TRPC6, and CD2AP are some of the key proteins that constitute the SD. Mutations in these proteins are implicated in nephrotic syndrome and congenital nephropathies which are characterised by heavy proteinuria. The mechanism of how mutations in these proteins predispose to proteinuria is not known. Furthermore, the structural details of proteins that constitute SD are largely unknown. In this study, we built models for nephrin, CD2AP, podocin, and TRPC6 followed by docking and molecular dynamics simulations of the complex of these proteins. We speculate that the interfacial residues of SD proteins form a macromolecular complex through intrinsically disordered regions thereby conferring architectural stability to the SD, which is critical for glomerular permselectivity.
机译:肾脏的肾小球过滤屏障(GFB)在预防大分子的排泄并确保形成超过滤尿液方面发挥了乐曲作用。巨粒细胞是GFB的必要组分,其为细肾小球毛细管提供上皮覆盖率。形成多粒细胞相邻脚工艺之间的唯一接触的狭缝 - 隔膜(SD)由多聚体蛋白质组件组成。 SD用作分子筛和赋予尺寸和电荷选择性屏障。 Nephrin,Podocin,TRPC6和CD2AP是构成SD的一些关键蛋白质。这些蛋白质中的突变涉及肾病综合征和先天性肾病,其特征在于重蛋白尿。这些蛋白质中突变如何易于蛋白尿的机制是未知的。此外,构成SD的蛋白质的结构细节在很大程度上是未知的。在这项研究中,我们为肾素,CD2AP,豆荚和TRPC6构建了模型,然后进行了这些蛋白质复合物的对接和分子动力学模拟。我们推测SD蛋白的界面残留物通过本质无序区域形成大分子复合物,从而赋予SD的建筑稳定性,这对于肾小球渗透性至关重要。

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