泛印度疾病队列和人口规模数据中的威尔逊病基因组图谱

IF 2.6 4区 医学 Q2 CLINICAL NEUROLOGY Movement Disorders Clinical Practice Pub Date : 2024-11-13 DOI:10.1002/mdc3.14266
Mukesh Kumar, Srishti Sharma, Sanjay Pandey, Geetha Mammayil, Aslam Pala Kuzhiyil, Srijaya Sreesh, Riyaz Arakkal, Divya M Radhakrishnan, Roopa Rajan, Deepak Amalnath, Reena Gulati, Naresh Tayade, Shine Sadasivan, Arun Valsan, Jagadeesh Menon, Mahesh Kamate, Sandeep Kumar Mathur, Radha Mahadevan, Bhavna Dhingra, Rajneesh Rajan, Kuldeep Singh, Shalimar, Suja K Geevarghese, Vikram S Kumar, John Menachery, Aminu Aliyar, Rahul C Bhoyar, Bani Jolly, Abhinav Jain, Arvinden Vittal Rangan, Trisha Moitra, Aditi Mhaske, Vishu Gupta, Vigneshwar Senthivel, Anushree Mishra, Arti Saini, Utkarsh Gaharwar, Sridhar Sivasubbu, Vinod Scaria, Binukumar B K
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引用次数: 0

摘要

背景:威尔逊氏病(WD)由致病性 ATP7B 基因变异引起,主要在肝、脑和肾中造成铜蓄积:在印度,尽管对 ATP7B 基因变异进行了研究,但威尔森氏病往往得不到诊断,其发病率、携带率和变异谱仍然未知:一项多中心研究通过全外显子测序检查了印度裔个体中 WD 的遗传变异。该研究使用了 InDelible 结构变异调用管道,并对 ATP7B AlphaFold 蛋白结构中意义不确定的变异(VUS)进行了分子动力学模拟。此外,还开发了一个针对 WD 的高通量基因筛选面板:本研究对 128 例临床诊断的 WD 病例进行了检查,发现 74 例基因确诊病例,其中 22 例有 ATP7B 变异,32 例无变异。研究发现了 22 个新型 ATP7B 基因变异,包括一个被归类为结构变异的 322 bp 缺失。分子动力学模拟突显了 11 个 ATP7B VUS 的潜在有害效应。基因负担分析表明与 ANO8、LGR4 和 CDC7 相关。确定了致病变异的 ATP7B 基因热点。患病率和携带率分别被确定为 18,678 分之一和 67 分之一。多重测序面板显示了准确诊断 WD 的前景:这项研究为了解印度 WD 的遗传变异和患病率提供了重要依据,解决了 WD 诊断不足的问题。它强调了 ATP7B 基因中的新型遗传变异、其他基因的参与、用于 WD 诊断和管理的可扩展、具有成本效益的多重测序面板,以及 WD 护理方面有望取得的进展。
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The Genomic Landscape of Wilson Disease in a Pan India Disease Cohort and Population-Scale Data.

Background: Wilson's disease (WD) results from pathogenic ATP7B gene variations, causing copper accumulation mainly in the liver, brain, and kidneys.

Objectives: In India, despite studies on ATP7B variants, WD often goes undiagnosed, with the prevalence, carrier rate, and mutation spectrum remaining unknown.

Methods: A multicenter study examined genetic variations in WD among individuals of Indian origin via whole exome sequencing. The study used the InDelible structural variants calling pipeline and conducted molecular dynamic simulations on variants of uncertain significance (VUS) in ATP7B AlphaFold protein structures. Additionally, a high-throughput gene screening panel for WD was developed.

Results: This study examined 128 clinically diagnosed cases of WD, revealing 74 genetically confirmed cases, 22 with ATP7B variants, and 32 without. Twenty-two novel ATP7B gene variants were identified, including a 322 bp deletion classified as a structural variant. Molecular dynamics simulations highlighted the potential deleterious effects of 11 ATP7B VUS. Gene burden analysis suggested associations with ANO8, LGR4, and CDC7. ATP7B gene hotspots for pathogenic variants were identified. Prevalence and carrier rates were determined as one in 18,678 and one in 67, respectively. A multiplex sequencing panel showed promise for accurate WD diagnosis.

Conclusions: This study offers crucial insights into WD's genetic variations and prevalence in India, addressing its underdiagnosis. It highlights the novel genetic variants in the ATP7B gene, the involvement of other genes, a scalable, cost-effective multiplex sequencing panel for WD diagnosis and management and promising advancements in WD care.

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来源期刊
CiteScore
4.00
自引率
7.50%
发文量
218
期刊介绍: Movement Disorders Clinical Practice- is an online-only journal committed to publishing high quality peer reviewed articles related to clinical aspects of movement disorders which broadly include phenomenology (interesting case/case series/rarities), investigative (for e.g- genetics, imaging), translational (phenotype-genotype or other) and treatment aspects (clinical guidelines, diagnostic and treatment algorithms)
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