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人类原弹性蛋白 rs2071307 多态性的进化背景和功能后果。

The evolutionary background and functional consequences of the rs2071307 polymorphism in human tropoelastin.

机构信息

Molecular Medicine Program, Research Institute, The Hospital for Sick Children, Toronto, Ontario, USA.

Elvesys Microfluidics Innovation Center, 172 rue de Charonne, 75011, Paris, France.

出版信息

Biopolymers. 2021 Feb;112(2):e23414. doi: 10.1002/bip.23414. Epub 2020 Dec 22.

DOI:10.1002/bip.23414
PMID:33351193
Abstract

Elastin is a major polymeric protein of the extracellular matrix, providing critical properties of extensibility and elastic recoil. The rs2071307 genomic polymorphism, resulting in the substitution of a serine for a glycine residue in a VPG motif in tropoelastin, has an unusually high minor allele frequency in humans. A consequence of such allelic heterozygosity would be the presence of a heterogeneous elastin polymer in up to 50% of the population, a situation which appears to be unique to Homo sapiens. VPG motifs are extremely common in hydrophobic domains of tropoelastins and are the sites of transient β-turns that are essential for maintaining the conformational flexibility required for its function as an entropic elastomer. Earlier data demonstrated that single amino acid substitutions in tropoelastin can have functional consequences for polymeric elastin, particularly when present in mixed polymers. Here, using NMR and molecular dynamics approaches, we show the rs2071307 polymorphism reduces local propensity for β-turn formation, with a consequent increase in polypeptide hydration and an expansion of the conformational ensemble manifested as an increased hydrodynamic radius, radius of gyration and asphericity. Furthermore, this substitution affects functional properties of polymeric elastin, particularly in heterogeneous polymers mimicking allelic heterozygosity. We discuss whether such effects, together with the unusually high minor allele frequency of the polymorphism, could imply some some evolutionary advantage for the heterozygous state.

摘要

弹性蛋白是细胞外基质的主要聚合蛋白,提供了伸展性和弹性回弹的关键特性。弹性蛋白原中 VPG 基序中的丝氨酸被甘氨酸取代的 rs2071307 基因组多态性,在人类中的次要等位基因频率异常高。这种等位基因杂合性的结果将是高达 50%的人群中存在异质弹性蛋白聚合物,这种情况似乎是智人所独有的。VPG 基序在原弹性蛋白的疏水区极其常见,是瞬时β-转角的位点,对于维持其作为熵弹性体的功能所需的构象灵活性至关重要。早期的数据表明,原弹性蛋白中的单个氨基酸取代可能对聚合弹性蛋白具有功能后果,特别是当存在于混合聚合物中时。在这里,我们使用 NMR 和分子动力学方法表明,rs2071307 多态性降低了局部形成β-转角的倾向,随之而来的是多肽水合作用增加,构象集合的扩展表现为水动力半径、回转半径和各向异性增加。此外,这种取代会影响聚合弹性蛋白的功能特性,特别是在模拟等位基因杂合性的异质聚合物中。我们讨论了这种影响,以及多态性的异常高的次要等位基因频率,是否可能意味着杂合状态存在一些进化优势。

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