与心血管特征相关的线粒体相关变异体。
Mitochondrial related variants associated with cardiovascular traits.
作者信息
Cañadas-Garre Marisa, Maqueda Joaquín J, Baños-Jaime Blanca, Hill Claire, Skelly Ryan, Cappa Ruaidhri, Brennan Eoin, Doyle Ross, Godson Catherine, Maxwell Alexander P, McKnight Amy Jayne
机构信息
Molecular Epidemiology and Public Health Research Group, Centre for Public Health, Queen's University Belfast, Institute for Clinical Sciences A, Royal Victoria Hospital, Belfast, United Kingdom.
MRC Integrative Epidemiology Unit, Bristol Medical School (Population Health Sciences), University of Bristol Oakfield House, Belfast, United Kingdom.
出版信息
Front Physiol. 2024 Aug 27;15:1395371. doi: 10.3389/fphys.2024.1395371. eCollection 2024.
INTRODUCTION
Cardiovascular disease (CVD) is responsible for over 30% of mortality worldwide. CVD arises from the complex influence of molecular, clinical, social, and environmental factors. Despite the growing number of autosomal genetic variants contributing to CVD, the cause of most CVDs is still unclear. Mitochondria are crucial in the pathophysiology, development and progression of CVDs; the impact of mitochondrial DNA (mtDNA) variants and mitochondrial haplogroups in the context of CVD has recently been highlighted.
AIMS
We investigated the role of genetic variants in both mtDNA and nuclear-encoded mitochondrial genes (NEMG) in CVD, including coronary artery disease (CAD), hypertension, and serum lipids in the UK Biobank, with sub-group analysis for diabetes.
METHODS
We investigated 371,542 variants in 2,527 NEMG, along with 192 variants in 32 mitochondrial genes in 381,994 participants of the UK Biobank, stratifying by presence of diabetes.
RESULTS
Mitochondrial variants showed associations with CVD, hypertension, and serum lipids. Mitochondrial haplogroup J was associated with CAD and serum lipids, whereas mitochondrial haplogroups T and U were associated with CVD. Among NEMG, variants within Nitric Oxide Synthase 3 () showed associations with CVD, CAD, hypertension, as well as diastolic and systolic blood pressure. We also identified Translocase Of Outer Mitochondrial Membrane 40 () variants associated with CAD; Solute carrier family 22 member 2 () variants associated with CAD and CVD; and variants associated with hypertension. Variants within these three genes were also associated with serum lipids.
CONCLUSION
Our study demonstrates the relevance of mitochondrial related variants in the context of CVD. We have linked mitochondrial haplogroup U to CVD, confirmed association of mitochondrial haplogroups J and T with CVD and proposed new markers of hypertension and serum lipids in the context of diabetes. We have also evidenced connections between the etiological pathways underlying CVDs, blood pressure and serum lipids, placing , , and genes as common nexuses.
引言
心血管疾病(CVD)导致全球超过30%的死亡率。CVD源于分子、临床、社会和环境因素的复杂影响。尽管导致CVD的常染色体遗传变异数量不断增加,但大多数CVD的病因仍不清楚。线粒体在CVD的病理生理学、发展和进展中起着关键作用;线粒体DNA(mtDNA)变异和线粒体单倍群在CVD背景下的影响最近受到了关注。
目的
我们在英国生物银行中研究了mtDNA和核编码线粒体基因(NEMG)中的遗传变异在CVD中的作用,包括冠状动脉疾病(CAD)、高血压和血脂,并对糖尿病进行了亚组分析。
方法
我们在英国生物银行的381,994名参与者中研究了2,527个NEMG中的371,542个变异,以及32个线粒体基因中的192个变异,并按是否患有糖尿病进行分层。
结果
线粒体变异与CVD、高血压和血脂有关。线粒体单倍群J与CAD和血脂有关,而线粒体单倍群T和U与CVD有关。在NEMG中,一氧化氮合酶3()内的变异与CVD、CAD、高血压以及舒张压和收缩压有关。我们还鉴定出与CAD相关的外线粒体膜转位酶40()变异;与CAD和CVD相关的溶质载体家族22成员2()变异;以及与高血压相关的变异。这三个基因内的变异也与血脂有关。
结论
我们的研究证明了线粒体相关变异在CVD背景下的相关性。我们将线粒体单倍群U与CVD联系起来,证实了线粒体单倍群J和T与CVD的关联,并提出了糖尿病背景下高血压和血脂的新标志物。我们还证明了CVD、血压和血脂潜在病因途径之间的联系,将、、和基因作为共同的联系点。
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