PHACTR1 and APOC1 genetic variants are associated with multi-vessel coronary artery disease.

IF 3.9 2区 医学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Cynthia Al Hageh, Siobhán O'Sullivan, Andreas Henschel, Antoine Abchee, Mireille Hantouche, Nantia Iakovidou, Taly Issa, Stephanie Chacar, Moni Nader, Pierre A Zalloua
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引用次数: 0

Abstract

Background: Severe coronary artery disease (CAD) represents an advanced arterial narrowing, often associated with critical complications like myocardial infarction and angina. This study aimed to comprehensively investigate determinants of severe and multi-vessel CAD manifestations.

Methods: One thousand nine hundred patients with severe and multivessel CAD (stenosis > 70%) were recruited along with 1,056 controls without stenosis. Associations using a genotyping panel comprising 159 Single Nucleotide Polymorphisms (SNPs) previously implicated in CAD pathogenesis were examined and these associations were replicated using the UK Biobank cohort (N = 29,970).

Results: The investigation identified 14 genetic associations with severe CAD, of which 7 were also associated with multivessel disease. Notably, PHACTR1 SNP (rs9349379*G) showed a higher association with severe and multivessel CAD in individuals aged ≤ 65, indicating a higher risk of early disease onset. Conversely, the APOC1/APOE SNP (rs445925*T) is associated with reduced susceptibility to severe CAD and multivessel disease in individuals aged over 65, indicating a persistent negative association.

Conclusions: Following replication of the associations in the large UK Biobank dataset, it was found that patients carrying the rs9349379*G variant in the PHACTR1 gene are at risk of developing severe or multivessel disease. Conversely, the rs445925*T variant in APOC1/APOE is associated with reduced susceptibility to severe CAD and multivessel disease, highlighting the significance of this genetic variant in these specific CAD presentations. This study contributes to a better understanding of CAD heterogeneity, paving the way for tailored management strategies based on genetic profiles.

PHACTR1 和 APOC1 基因变异与多血管冠状动脉疾病有关。
背景:严重的冠状动脉疾病(CAD)代表着晚期动脉狭窄,通常与心肌梗死和心绞痛等严重并发症相关。本研究旨在全面调查严重和多支冠状动脉疾病表现的决定因素:招募了 1900 名重度多血管 CAD 患者(血管狭窄程度大于 70%)和 1056 名无血管狭窄的对照者。使用由 159 个先前与 CAD 发病机制有关的单核苷酸多态性(SNPs)组成的基因分型小组对这些关联进行了研究,并使用英国生物库队列(N = 29,970 人)对这些关联进行了复制:结果:调查发现了 14 个与严重 CAD 相关的基因,其中 7 个还与多血管疾病相关。值得注意的是,PHACTR1 SNP(rs9349379*G)在年龄小于 65 岁的人群中与严重和多血管 CAD 的关联度较高,表明早期发病的风险较高。相反,APOC1/APOE SNP(rs445925*T)与 65 岁以上人群对严重 CAD 和多血管疾病的易感性降低有关,表明两者之间存在持续的负相关:结论:在英国生物库大型数据集中复制相关性后发现,携带 PHACTR1 基因 rs9349379*G 变异的患者有罹患严重或多血管疾病的风险。相反,APOC1/APOE 基因中的 rs445925*T 变体与严重 CAD 和多血管疾病的易感性降低有关,这突显了该基因变体在这些特定 CAD 表现中的重要性。这项研究有助于更好地了解 CAD 的异质性,为根据遗传特征制定有针对性的管理策略铺平了道路。
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来源期刊
Lipids in Health and Disease
Lipids in Health and Disease 生物-生化与分子生物学
CiteScore
7.70
自引率
2.20%
发文量
122
审稿时长
3-8 weeks
期刊介绍: Lipids in Health and Disease is an open access, peer-reviewed, journal that publishes articles on all aspects of lipids: their biochemistry, pharmacology, toxicology, role in health and disease, and the synthesis of new lipid compounds. Lipids in Health and Disease is aimed at all scientists, health professionals and physicians interested in the area of lipids. Lipids are defined here in their broadest sense, to include: cholesterol, essential fatty acids, saturated fatty acids, phospholipids, inositol lipids, second messenger lipids, enzymes and synthetic machinery that is involved in the metabolism of various lipids in the cells and tissues, and also various aspects of lipid transport, etc. In addition, the journal also publishes research that investigates and defines the role of lipids in various physiological processes, pathology and disease. In particular, the journal aims to bridge the gap between the bench and the clinic by publishing articles that are particularly relevant to human diseases and the role of lipids in the management of various diseases.
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