Analysis of 272 Genetic Variants in the Upgraded Interactive FXI Web Database Reveals New Insights into FXI Deficiency.

TH Open: Companion Journal to Thrombosis and Haemostasis Pub Date : 2021-11-01 eCollection Date: 2021-10-01 DOI:10.1055/a-1683-8605
Victoria A Harris, Weining Lin, Stephen J Perkins
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引用次数: 5

Abstract

Coagulation Factor XI (FXI) is a plasma glycoprotein composed of four apple (Ap) domains and a serine protease (SP) domain. FXI circulates as a dimer and activates Factor IX (FIX), promoting thrombin production and preventing excess blood loss. Genetic variants that degrade FXI structure and function often lead to bleeding diatheses, commonly termed FXI deficiency. The first interactive FXI variant database underwent initial development in 2003 at https://www.factorxi.org . Here, based on a much improved FXI crystal structure, the upgraded FXI database contains information regarding 272 FXI variants (including 154 missense variants) found in 657 patients, this being a significant increase from the 183 variants identified in the 2009 update. Type I variants involve the simultaneous reduction of FXI coagulant activity (FXI:C) and FXI antigen levels (FXI:Ag), whereas Type II variants result in decreased FXI:C yet normal FXI:Ag. The database updates now highlight the predominance of Type I variants in FXI. Analysis in terms of a consensus Ap domain revealed the near-uniform distribution of 81 missense variants across the Ap domains. A further 66 missense variants were identified in the SP domain, showing that all regions of the FXI protein were important for function. The variants clarified the critical importance of changes in surface solvent accessibility, as well as those of cysteine residues and the dimer interface. Guidelines are provided below for clinicians who wish to use the database for diagnostic purposes. In conclusion, the updated database provides an easy-to-use web resource on FXI deficiency for clinicians.

对升级的交互式FXI网络数据库中272个遗传变异的分析揭示了对FXI缺陷的新见解。
FXI作为二聚体循环,激活因子IX (FIX),促进凝血酶的产生,防止过量失血。降低FXI结构和功能的基因变异经常导致出血性糖尿病,通常称为FXI缺乏症。第一个交互式FXI变体数据库于2003年在https://www.factorxi.org进行了初步开发。在此,基于大大改进的FXI晶体结构,升级后的FXI数据库包含了657名患者中发现的272个FXI变体(包括154个错义变体)的信息,这比2009年更新中发现的183个变体有了显著增加。I型变异涉及FXI凝血剂活性(FXI:C)和FXI抗原水平(FXI:Ag)的同时降低,而II型变异导致FXI:C降低而FXI:Ag正常。数据库更新现在突出了I型变异在FXI中的优势。根据一致的Ap结构域进行分析,发现81个错义变异在Ap结构域的分布近乎均匀。在SP结构域中还发现了66个错义变体,这表明FXI蛋白的所有区域对功能都很重要。这些变化阐明了表面溶剂可及性变化的重要性,以及半胱氨酸残基和二聚体界面的变化。为希望使用该数据库进行诊断的临床医生提供以下指南。总之,更新后的数据库为临床医生提供了一个易于使用的关于FXI缺乏的网络资源。
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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