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Hypertension is associated with a variant in the RARRES2 gene in populations of Ouro Preto Minas Gerais Brazil: a cross-sectional study

机译:高血压与RARRES2基因的变种有关在巴西米纳斯吉拉斯米纳斯Gerais群体中的RARRES2基因中的变种:横断面研究

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摘要

Background: Arterial hypertension (AH) is implicated in vascular health and contributes significantly to cardiovascular morbidity and mortality. In addition to the contribution of usual risk factors for AH, elucidating the influence of genetic factors is a promising area of investigation. Therefore, we evaluated the association between AH and cardiovascular risk factors (CVRFs) and genetic polymorphisms in communities in Southeast Brazil. Methods: A total of 515 adults aged 18-91 years, who were cross-sectionally assessed between 2015-2016, were included. Demographic, clinical, behavioral, anthropometric characteristics, and laboratory parameters and 12 single nucleotide polymorphisms in seven candidate genes involved in cardiovascular risk (RARRES2, AGT, NOS3, GNB3, APOE, APOB, APOC3, LDLR, and PPARG) were evaluated, with AH as the outcome. Sex, age, and laboratory parameters were considered the main confounding factors. Results: There was a significant association between age >60 years (odds ratio [OR] =6.74), alcohol dependence (OR=3.84), smoking (OR=1.74), overweight (OR=1.74), high plasma triglyceride (TG) levels (OR=1.98) and low high-density lipoprotein (HDL-c) (OR=6.22), diabetes (OR=3.68), and insulin resistance (OR=2.40) and AH. A significant association was observed between rs4721 in RARRES2 and AH. The T allele in homozygosis was a potent chance modifier for AH. The highest chance gradients for AH were characterized by the presence of the TT genotype and DMT2 (OR=9.70), high TG (OR=6.26), low HDL-c (OR=8.20), and age more than 60 years (OR=9.96). Conclusion: The interaction of the T allele of the rs4721 polymorphism in RARRES2 with CVRFs may predispose carriers to a higher cardiovascular risk.
机译:背景:动脉高血压(AH)在血管健康,并有助于牵连显著心血管发病率和死亡率。除了通常的危险因素贡献AH,阐明遗传因素的影响调查的有希望的领域。因此,我们评估AH和心血管危险因素(CVRFs)和遗传多态性之间的关联,在巴西东南部的社区。方法:共有515名成人年龄18-91年,谁是截面为2015 - 2016年之间的评估,都包括在内。人口学,临床医学,行为科学,人体特征和实验室参数和参与心血管疾病的危险7候选基因12个单核苷酸多态性(RARRES2,AGT,NOS3,GNB3,APOE,APOB,APOC3,LDLR和PPARG)进行了评价,与AH作为结局。性别,年龄,和实验室参数进行考虑的主要干扰因素。结果:年龄之间(= 1.74 OR)(= 1.74 OR)一个显著关联> 60岁(比值比[OR] = 6.74),酒精依赖(OR = 3.84),吸烟,超重,高血浆甘油三酯(TG)水平(OR = 1.98)和低高密度脂蛋白(HDL-C)(OR = 6.22),糖尿病(OR = 3.68),和胰岛素抵抗(OR = 2.40)和AH。在RARRES2和AH rs4721之间观察到显著相关性。在纯合的T等位基因是为AH的有力机会修正。由TT基因型和DMT2(OR = 9.70),高TG(OR = 6.26),低HDL-C(OR = 8.20),和年龄60岁以上的存在AH最高机会梯度进行了表征(OR = 9.96)。结论:RARRES2的rs4721多态性与CVRFs的T等位基因的相互作用可能使运营商以更高的心血管风险。

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