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Association of three-gene interaction among MTHFR, ALOX5AP and NOTCH3 with thrombotic stroke: a multicenter case–control study

机译:MTHFR,ALOX5AP和NOTCH3之间的三基因相互作用与血栓性卒中的关联:多中心病例对照研究

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摘要

Stroke is a common complex trait and does not follow Mendelian pattern of inheritance. Gene–gene or gene–environment interactions may be responsible for the complex trait. How the interactions contribute to stroke is still under research. This study aimed to explore the association between gene–gene interactions and stroke in Chinese in a large case–control study. Nearly 4,000 participants were recruited from seven clinical centers. Eight variants in five candidate genes were examined for stroke risk. Gene–gene interactions were explored by using Generalized Multifactor Dimensionality Reduction (GMDR). A significant gene–gene interaction was found by GMDR. The best model including MTHFR C677T, ALOX5AP T2354A and NOTCH3 C381T scored 10 for Cross-Validation Consistency and 9 for Sign Test (P = 0.0107). The individuals with combination of MTHFR 677TT, ALOX5AP 2354AA and NOTCH3 381TT/TC had a significantly higher risk of thrombotic stroke (OR 3.165, 95% CI 1.461–6.858, P = 0.003). Our results show that combination of these alleles conferred higher risk for stroke than single risk allele. The gene–gene interaction may serve as a novel area for stroke research. The three-locus combination may change the susceptibility of particular subjects to the disease.
机译:中风是一个常见的复杂特征,并不遵循孟德尔的遗传模式。基因-基因或基因-环境的相互作用可能是造成复杂性状的原因。相互作用如何导致中风仍在研究中。这项研究的目的是在一个大型病例对照研究中探讨中国人基因与基因的相互作用与中风之间的关系。从七个临床中心招募了近4,000名参与者。检查了五个候选基因中的八个变体的中风风险。通过使用广义多因素降维(GMDR)探索了基因与基因之间的相互作用。 GMDR发现了重要的基因-基因相互作用。包括MTHFR C677T,ALOX5AP T2354A和NOTCH3 C381T在内的最佳模型的交叉验证一致性得分为10,而符号测试得分为9(P = 0.0107)。结合使用MTHFR 677TT,ALOX5AP 2354AA和NOTCH3 381TT / TC的个体发生血栓性中风的风险明显更高(OR 3.165,95%CI 1.461–6.858,P = 0.003)。我们的结果表明,这些等位基因的组合比单风险等位基因具有更高的中风风险。基因与基因的相互作用可能成为卒中研究的新领域。三位点组合可能会改变特定受试者对疾病的敏感性。

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