Known pathogenic gene variants and new candidates detected in Sudden Unexpected Infant Death using Whole Genome Sequencing.

medRxiv : the preprint server for health sciences Pub Date : 2023-11-29 DOI:10.1101/2023.09.11.23295207

Angela M Bard, Lindsay V Clark, Erdal Cosgun, Kimberly A Aldinger, Andrew Timms, Lely A Quina, Juan M Lavista Ferres, David Jardine, Elisabeth A Haas, Tatiana M Becker, Chelsea M Pagan, Avni Santani, Diego Martinez, Soumitra Barua, Zakkary McNutt, Addie Nesbitt, Edwin A Mitchell, Jan-Marino Ramirez

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Abstract

Purpose: To gain insights into potential genetic factors contributing to the infant's vulnerability to Sudden Unexpected Infant Death (SUID).

Methods: Whole Genome Sequencing (WGS) was performed on 145 infants that succumbed to SUID, and 576 healthy adults. Variants were filtered by gnomAD allele frequencies and predictions of functional consequences.

Results: Variants of interest were identified in 86 genes, 63.4% of our cohort. Seventy-one of these have been previously associated with SIDS/SUID/SUDP. Forty-three can be characterized as cardiac genes and are related to cardiomyopathies, arrhythmias, and other conditions. Variants in 22 genes were associated with neurologic functions. Variants were also found in 13 genes reported to be pathogenic for various systemic disorders. Variants in eight genes are implicated in the response to hypoxia and the regulation of reactive oxygen species (ROS) and have not been previously described in SIDS/SUID/SUDP. Seventy-two infants met the triple risk hypothesis criteria (Figure 1).

Conclusion: Our study confirms and further expands the list of genetic variants associated with SUID. The abundance of genes associated with heart disease and the discovery of variants associated with the redox metabolism have important mechanistic implications for the pathophysiology of SUID.

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使用全基因组测序（WGS）在婴儿猝死（SUID）中检测到的已知致病基因变体和新的候选基因。

目的：在这项研究中，我们对出生第一年死于SUID的儿童进行了WGS，以深入了解可能导致婴儿易受这种悲惨结果影响的潜在遗传风险因素。方法：对145例SUID病例和576例健康成人对照进行全基因组测序。通过gnomAD等位基因频率和使用计算工具对功能后果的预测来过滤变异。结果：在63.4%的队列中，我们在86个基因中发现了156个感兴趣的变体，其中71个基因中有128个罕见/超罕见变体，这些变体以前与SIDS/SUID/SUDP相关。在43个可被表征为心脏基因的基因中发现了88个变体，这些变体以前与心肌病、Brugada和长QT综合征等有关。在先前报道的SIDS/SUID/SUDP中的22个基因中也发现了29个与神经功能相关的变异。据报道，在13个对各种系统性疾病具有致病性的基因中发现了19种变异，其中11种发生在6个先前在SIDS/SUID/SUDP中描述的基因中，8个没有。我们还发现了8个基因中的20个变体，这些变体与缺氧反应和活性氧（ROS）的调节有关，而以前在SIDS/SUID/SUDP中没有描述过。结论：我们的研究证实并进一步扩展了与SUID相关的遗传变体列表。与心脏病相关的基因的丰富和与氧化还原代谢相关的变体的发现对SUID的病理生理学具有重要的机制意义。

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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medRxiv : the preprint server for health sciences

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