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AGT 和 NOS3 基因多态性与传统危险因素的相互作用增加了高血压的易感性。

The interaction of AGT and NOS3 gene polymorphisms with conventional risk factors increases predisposition to hypertension.

机构信息

1Institute of Genetics and Biochemistry, Federal University of Uberlândia, Brazil.

出版信息

J Renin Angiotensin Aldosterone Syst. 2013 Dec;14(4):360-8. doi: 10.1177/1470320312452027. Epub 2012 Jul 12.

Abstract

Renin-angiotensin and kallikrein-kinin systems are interconnected, regulating blood pressure homeostasis. We have demonstrated the interactions among polymorphisms of the angiotensinogen (AGT) and endothelial nitric oxide synthase (NOS3) genes and conventional risk factors affecting the hypertension occurrence. Individuals were recruited (n=192) and classified into hypertensive (HG; n=140) and normotensive (NG; n=52) groups. The genotypic distribution of the Met235Thr (AGT) and Glu298Asp (NOS3) polymorphisms demonstrated that both are independent risk factors of hypertension (p=0.02 and p=0.008, respectively). The concomitant presence of these polymorphisms in the HG group was significantly different (p=0.001) from the NG. Both gene polymorphisms presented an additive effect for the unfavourable alleles T and A, respectively, and 95% of the double mutant homozygotes were classified into the HG. Specific interactions among certain conventional factors and the presence of at least one unfavourable allele presented significant odds towards hypertension. Blood pressure homeostasis was affected by genetic polymorphisms conditioned by the T and A alleles of the AGT and NOS3 genes, respectively, which acted independently. However, their interaction with smoking, sedentariness, age and total cholesterol may have increased the predisposition to hypertension, which may explain most of the hypertension cases.

摘要

肾素-血管紧张素和激肽-缓激肽系统相互关联,调节血压的稳态。我们已经证明了血管紧张素原(AGT)和内皮型一氧化氮合酶(NOS3)基因的多态性与影响高血压发生的常规危险因素之间的相互作用。我们招募了个体(n=192)并将其分为高血压组(HG;n=140)和正常血压组(NG;n=52)。Met235Thr(AGT)和Glu298Asp(NOS3)多态性的基因型分布表明,这两种多态性都是高血压的独立危险因素(p=0.02 和 p=0.008)。这两种基因多态性在 HG 组中的同时存在差异显著(p=0.001)。这两种基因多态性对不利等位基因 T 和 A 分别呈现出相加效应,并且 95%的双突变纯合子被归入 HG。某些常规因素的特定相互作用以及至少存在一个不利等位基因的存在与高血压显著相关。血压稳态受到由 AGT 和 NOS3 基因的 T 和 A 等位基因分别条件的遗传多态性的影响,它们独立作用。然而,它们与吸烟、久坐、年龄和总胆固醇的相互作用可能增加了患高血压的倾向,这可能解释了大多数高血压病例。

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