血管紧张素i转换酶基因插入/缺失多态性与风湿性心脏病风险的关系

Hsiang-Tai Chou, Chang-Hai Tsai, Fuu-Jen Tsai
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引用次数: 25

摘要

风湿性心脏病(RHD)患者的二尖瓣或主动脉瓣的持续创伤可能是由闷烧的风湿病过程和湍流对二尖瓣或主动脉瓣的持续创伤共同作用造成的。有研究表明,血管紧张素i转换酶(ACE)可能在RHD发病过程中导致瓣膜纤维化和钙化增加。然而,ACE基因变异在RHD中的作用尚未在台湾大陆人群中进行研究。因此,我们开展了一项病例对照研究,探讨ACE基因插入/缺失(I/D)和G2350A多态性与RHD的可能关系。研究了115例超声心动图记录的RHD患者和100例年龄和性别匹配的正常对照。采用聚合酶链反应限制性内切法鉴定ACE基因I/D和G2350A多态性。RHD患者与正常对照组ACE I/D基因型分布(P = 0.02)和等位基因频率(P = 0.04)差异有统计学意义。与ACE I/D II基因型相关的RHD风险的优势比为2.12 (95% CI, 1.21-3.71)。与ACE I等位基因相关的RHD风险的优势比为1.50 (95% CI, 1.02-2.21)。ACE G2350A多态性与RHD无相关性(P = 0.90)。进一步将RHD患者分为二尖瓣疾病和联合瓣膜疾病亚组,两个亚组之间比较,这些基因多态性无统计学差异。本研究表明,ACE II基因型和I等位基因频率较高,支持ACE I/D基因多态性在台湾华人RHD发病风险中的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Association between angiotensin I-converting enzyme gene insertion/deletion polymorphism and risk of rheumatic heart disease.

Scarring and collagen deposition in the valves and destruction of myocytes may result from the combined effects of a smoldering rheumatic process and a constant trauma to the mitral valve or aortic valve by the turbulent flow in rheumatic heart disease (RHD). It has been suggested that angiotensin I-converting enzyme (ACE) may be responsible for the increased valvular fibrosis and calcification in the pathogenesis of RHD. However, the role of ACE genetic variant in RHD has not been studied among the Chinese population in Taiwan. Hence, a case-controlled study was carried out to investigate the possible relationship between the ACE gene insertion/deletion (I/D) and G2350A polymorphisms and RHD. A group of 115 patients with RHD documented by echocardiography and 100 age- and sex-matched normal control subjects were studied. ACE gene I/D and G2350A polymorphisms were identified by polymerase chain reaction-based restriction analysis. There was a significant difference in the distribution of ACE I/D genotypes (P = 0.02) and allelic frequencies (P = 0.04) between RHD cases and normal controls. An odds ratio for the risk of RHD associated with the ACE I/D II genotype was 2.12 (95% CI, 1.21-3.71). An odds ratio for the risk of RHD associated with the ACE I allele was 1.50 (95% CI, 1.02-2.21). The ACE G2350A polymorphism showed no association with RHD (P = 0.90). Further categorization of RHD patients into mitral valve disease and combined valve disease subgroups revealed no statistical difference in these gene polymorphisms when compared between the two subgroups. This study shows that patients with RHD have a higher frequency of ACE II genotype and I allele, which supports a role for ACE I/D gene polymorphisms in determining the risk of RHD in Taiwan Chinese.

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