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首页> 外文期刊>Journal of biophysics >Analysis of the REJ Module of Polycystin-1 Using Molecular Modeling and Force-Spectroscopy Techniques
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Analysis of the REJ Module of Polycystin-1 Using Molecular Modeling and Force-Spectroscopy Techniques

机译:分子建模和力谱技术分析多囊藻蛋白1的REJ模块

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Polycystin-1 is a large transmembrane protein, which, whenmutated, causes autosomal dominant polycystic kidney disease, one of the most common life-threatening genetic diseases that is a leading cause of kidney failure. The REJ (receptor for egg lelly) module is a major component of PC1 ectodomain that extends to about 1000 amino acids. Many missense disease-causing mutations map to this module; however, very little is known about the structure or function of this region. We used a combination of homology molecularmodeling, protein engineering, steered molecular dynamics (SMD) simulations, and single-molecule force spectroscopy (SMFS) to analyze the conformation and mechanical stability of the first ~420 amino acids of REJ. Homology molecular modeling analysis revealed that this region may contain structural elements that have an FNIII-like structure, which we named REJd1, REJd2, REJd3, and REJd4.We found that REJd1 has a highermechanical stability than REJd2 (~190 pN and 60 pN, resp.). Our data suggest that the putative domains REJd3 and REJd4 likely do not form mechanically stable folds. Our experimental approach opens a new way to systematically study the effects of disease-causing mutations on the structure and mechanical properties of the REJ module of PC1.
机译:Polycystin-1是一种大型跨膜蛋白,突变后会导致常染色体显性遗传多囊肾,这是最常见的威胁生命的遗传疾病之一,是导致肾衰竭的主要原因。 REJ(蛋l的受体)模块是PC1胞外域的主要组成部分,延伸至约1000个氨基酸。许多导致疾病的错义突变都映射到该模块。然而,对该区域的结构或功能知之甚少。我们结合了同源分子模型,蛋白质工程,分子导向动力学(SMD)模拟和单分子力谱分析(SMFS),分析了REJ的前420个氨基酸的构象和机械稳定性。同源分子模型分析表明,该区域可能包含具有FNIII样结构的结构元素,我们将其命名为REJd1,REJd2,REJd3和REJd4。我们发现REJd1具有比REJd2更高的机械稳定性(〜190 pN和60 pN,分别)。我们的数据表明推定域REJd3和REJd4可能不会形成机械稳定的褶皱。我们的实验方法为系统研究致病突变对PC1 REJ模块的结构和机械性能的影响开辟了一条新途径。

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