Analysis of 363 Genetic Variants in F5 via an Interactive Web Database Reveals New Insights into FV Deficiency and FV Leiden.

Christos Efthymiou, Emily H T Print, Anna Simmons, Stephen J Perkins
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Abstract

The inherited bleeding disorder Factor V (FV) deficiency and clotting risk factor FV Leiden are associated with genetic variants in the F5 gene. FV deficiency occurs with mild, moderate, severe, or asymptomatic phenotypes, and either dysfunctional or reduced amounts of plasma FV protein. Here we present an interactive web database containing 363 unique F5 variants derived from 801 patient records, with 199 FV deficiency-associated variants from 245 patient records. Their occurrence is rationalized based on the 2,224 residue sequence and new FV protein structures. The 199 FV deficiency variants correspond to 26 (13%) mild, 22 (11%) moderate, 49 (25%) severe, 35 (18%) asymptomatic, and 67 (34%) unreported phenotypes. Their variant distributions in the FV domains A1, A2, A3, B, C1 and C2 were 28 (14%), 32 (16%), 34 (17%), 42 (21%), 16 (8%), and 19 variants (10%), respectively, showing that these six regions contain similar proportions of variants. Variants associated with FV deficiency do not cluster near known protein-partner binding sites, thus the molecular mechanism leading to the phenotypes cannot be explained. However, the widespread distribution of FV variants in combination with a high proportion of buried variant residues indicated that FV is susceptible to disruption by small perturbations in its globular structure. Variants located in the disordered B domain also appear to disrupt the FV structure. We discuss how the interactive database provides an online resource that clarifies the clinical understanding of FV deficiency.

通过交互式Web数据库分析F5基因363个遗传变异,揭示FV缺乏症和FV莱顿病的新认识。
遗传性出血性疾病因子V (FV)缺乏和凝血危险因子FV Leiden与F5基因的遗传变异有关。FV缺乏症表现为轻度、中度、重度或无症状表型,血浆FV蛋白功能失调或减少。在这里,我们提出了一个交互式网络数据库,其中包含来自801例患者记录的363个独特的F5变异,以及来自245例患者记录的199个FV缺陷相关变异。根据2,224个残基序列和新的FV蛋白结构对其发生进行了合理化分析。199个FV缺陷变异对应于26个(13%)轻度,22个(11%)中度,49个(25%)重度,35个(18%)无症状,67个(34%)未报告的表型。它们在FV结构域A1、A2、A3、B、C1和C2的变异分布分别为28个(14%)、32个(16%)、34个(17%)、42个(21%)、16个(8%)和19个(10%),说明这6个区域的变异比例相近。与FV缺陷相关的变异不会聚集在已知的蛋白质伴侣结合位点附近,因此导致表型的分子机制无法解释。然而,FV变体的广泛分布以及高比例的埋藏变体残留物表明,FV很容易受到其球状结构中的微小扰动的破坏。位于无序B结构域的变异似乎也会破坏FV结构。我们讨论交互式数据库如何提供在线资源,以澄清FV缺陷的临床认识。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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