CSIR Institute of Genomics and Integrative Biology, Mathura Road, Delhi, 110 025, India.
Academy of Scientific and Innovative Research, CSIR-IGIB South Campus, Mathura Road, Delhi, India.
Sci Rep. 2020 Jun 3;10(1):9037. doi: 10.1038/s41598-020-66099-2.
Wilson disease (WD) is one of the most prevalent genetic diseases with an estimated global carrier frequency of 1 in 90 and a prevalence of 1 in 30,000. The disease owes its genesis to Kinnier Wilson who described the disease, and is caused by accumulation of Copper (Cu) in various organs including the liver, central nervous system, cornea, kidney, joints and cardiac muscle which contribute to the characteristic clinical features of WD. A number of studies have reported genetic variants in the ATP7B gene from diverse ethnic and geographical origins. The recent advent of next-generation sequencing approaches has also enabled the discovery of a large number of novel variants in the gene associated with the disease. Previous attempts have been made to compile the knowledgebase and spectrum of genetic variants from across the multitude of publications, but have been limited by the utility due to the significant differences in approaches used to qualify pathogenicity of variants in each of the publications. The recent formulation of guidelines and algorithms for assessment of the pathogenicity of variants jointly put forward by the American College of Medical Genetics and the Association of Molecular Pathologists (ACMG &) has provided a framework for evidence based and systematic assessment of pathogenicity of variants. In this paper, we describe a comprehensive resource of genetic variants in ATP7B gene manually curated from literature and data resources and systematically annotated using the ACMG & AMP guidelines for assessing pathogenicity. The resource therefore serves as a central point for clinicians and geneticists working on WD and to the best of our knowledge is the most comprehensive and only clinically annotated resource for WD. The resource is available at URL http://clingen.igib.res.in/WilsonGen/. We compiled a total of 3662 genetic variants from publications and databases associated with WD. Of these variants compiled, a total of 1458 were found to be unique entries. This is the largest WD database comprising 656 pathogenic/likely pathogenic variants reported classified according to ACMG & AMP guidelines. We also mapped all the pathogenic variants corresponding to ATP7B protein from literature and other databases. In addition, geographical origin and distribution of ATP7B pathogenic variants reported are also mapped in the database.
威尔逊病(WD)是最常见的遗传疾病之一,据估计全球携带者频率为 1/90,患病率为 1/30000。该疾病得名于 Kinnier Wilson,他描述了该疾病,并由铜(Cu)在包括肝脏、中枢神经系统、角膜、肾脏、关节和心肌在内的各种器官中的积累引起,这导致了 WD 的特征性临床特征。许多研究报告了来自不同种族和地理起源的 ATP7B 基因中的遗传变异。最近,下一代测序方法的出现也使得能够发现与该疾病相关的大量新基因变异。以前曾试图从众多出版物中汇编知识库和遗传变异谱,但由于每个出版物中用于确定变异致病性的方法存在显著差异,因此受到限制。美国医学遗传学学院和分子病理学家协会(ACMG &)联合提出的评估变异致病性的指南和算法的最新制定,为基于证据和系统地评估变异的致病性提供了一个框架。在本文中,我们描述了从文献和数据资源中手动整理的 ATP7B 基因遗传变异的综合资源,并使用 ACMG & 指南系统地注释了评估致病性的方法。因此,该资源可作为从事 WD 工作的临床医生和遗传学家的中心点,据我们所知,它是最全面的、唯一的临床注释 WD 资源。该资源可在 URL http://clingen.igib.res.in/WilsonGen/ 上获得。我们从与 WD 相关的出版物和数据库中总共编译了 3662 个遗传变异。在这些编译的变异中,共有 1458 个是唯一的条目。这是最大的 WD 数据库,包含根据 ACMG & 指南报告的 656 种致病性/可能致病性变异。我们还从文献和其他数据库中映射了所有与 ATP7B 蛋白对应的致病性变异。此外,数据库中还映射了报告的 ATP7B 致病性变异的地理起源和分布。
