Genetic variants associated with cardiac hypertrophy-related sudden cardiac death and cardiovascular outcomes in a Finnish population.

IF 5.1 2区 医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS Heart Pub Date : 2024-12-23 DOI:10.1136/heartjnl-2024-324623
Anne Doedens, Sini Skarp, Lauri Holmström, Lasse Pakanen, Samu Saarimäki, Risto Kerkelä, Katri Pylkäs, Heikki V Huikuri, Juhani Junttila
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Abstract

Background: Hypertrophic cardiomyopathy is a common cause of non-ischaemic sudden cardiac death (SCD). Left ventricular hypertrophy (LVH) without cardiomyopathy-related myocardial disarray is a common autopsy finding and is often associated with prior hypertension in SCD subjects. Our aim was to investigate novel rare gene variants among SCD subjects with presumably hypertension-related LVH and myocardial fibrosis at autopsy.

Methods: Whole exome sequencing was used to study rare variants (minor allele frequency<0.005) estimated to be deleterious in 96 non-ischaemic SCD subjects with presumably hypertension-related LVH and myocardial fibrosis. Associations of the identified variants with cardiac disease endpoints were replicated in the Finnish national genetic study (FinnGen) dataset.

Results: 18 variants were estimated likely to affect protein function and 14 of these were associated with cardiomyopathies, heart failure, conduction abnormalities, hypertension and/or cardiac arrest in Finnish population (FinnGen). Three of the variants were classified as pathogenic or likely pathogenic. These include the splice site variant NM_000449.3:c.234-1G>A in regulatory factor X5 and frameshift variants NM_000449.3:c.234-1G>A in dehydrogenase/reductase 7C and NM_015873.3:c.1164del in villin like.

Conclusions: We identified rare deleterious variants associated with LVH in SCD subjects. Several of the identified rare variants associated with cardiovascular endpoints including heart failure, cardiomyopathies, cardiac arrest and hypertension in general population.

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芬兰人群中与心脏肥大相关的心源性猝死和心血管后果有关的基因变异。
背景:肥厚型心肌病是导致非缺血性心脏性猝死(SCD)的常见原因。左心室肥厚(LVH)而无心肌病相关的心肌结构紊乱是常见的尸检发现,并且通常与 SCD 受试者之前患有高血压有关。我们的目的是研究尸检时推测与高血压相关的 LVH 和心肌纤维化的 SCD 受试者中的新型罕见基因变异:方法:采用全外显子组测序研究罕见变异(小等位基因频率):据估计,18个变异体可能会影响蛋白质功能,其中14个与芬兰人群(FinnGen)中的心肌病、心力衰竭、传导异常、高血压和/或心脏骤停有关。其中三个变异被归类为致病或可能致病。这些变异包括调节因子 X5 中的剪接位点变异 NM_000449.3:c.234-1G>A,脱氢酶/还原酶 7C 中的移帧变异 NM_000449.3:c.234-1G>A 和类似绒毛蛋白中的 NM_015873.3:c.1164del:我们发现了与 SCD 受试者 LVH 相关的罕见有害变异。结论:我们在 SCD 受试者中发现了与左心室肥厚相关的罕见致病变异,其中一些变异与心血管终点有关,包括心力衰竭、心肌病、心脏骤停和普通人群中的高血压。
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来源期刊
Heart
Heart 医学-心血管系统
CiteScore
10.30
自引率
5.30%
发文量
320
审稿时长
3-6 weeks
期刊介绍: Heart is an international peer reviewed journal that keeps cardiologists up to date with important research advances in cardiovascular disease. New scientific developments are highlighted in editorials and put in context with concise review articles. There is one free Editor’s Choice article in each issue, with open access options available to authors for all articles. Education in Heart articles provide a comprehensive, continuously updated, cardiology curriculum.
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