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Genotype-by-sex interaction on fasting insulin concentration: the HyperGEN study.

机译:空腹胰岛素浓度的基因型-性别相互作用:HyperGEN研究。

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Recent studies have demonstrated the importance of sex effects on the underlying genetic architecture of insulin-related traits. To explore sex-specific genetic effects on fasting insulin, we tested for genotype-by-sex interaction and conducted linkage analysis of fasting insulin in Hypertension Genetic Epidemiology Network families. Hypertensive siblings and their first-degree relatives were recruited from five field centers. We performed a genome scan for quantitative trait loci influencing fasting insulin among 1,505 European Americans and 1,616 African Americans without diabetes. Sex-stratified linear regression models, adjusted for race, center, and age, were explored. The Mammalian Genotyping Service typed 391 microsatellite markers, spaced roughly 9 cM. Variance component linkage analysis was performed in SOLAR using ethnic-specific marker allele frequencies and multipoint IBDs calculated in MERLIN. We detected a quantitative trait locus influencing fasting insulin in female subjects (logarithm of odds [LOD] = 3.4) on chromosome 2 at 95 cM (between GATA69E12 and GATA71G04) but not in male subjects (LOD = 0.0, P for interaction = 0.007). This sex-specific signal at 2p13.2 was detected in both European-American (LOD = 2.1) and African-American (LOD = 1.2) female subjects. Our findings overlap with several other linkage reports of insulin-related traits and demonstrate the importance of considering complex context-dependent interactions in the search for insulin-related genes.
机译:最近的研究表明性别影响对胰岛素相关性状的潜在遗传结构的重要性。为了探讨对空腹胰岛素的性别特异性遗传效应,我们测试了性别与性别之间的相互作用,并在高血压遗传流行病学网络家族中进行了空腹胰岛素的连锁分析。高血压兄弟姐妹及其一级亲属是从五个现场中心招募的。我们进行了基因组扫描,以分析影响1,505例欧洲裔美国人和1,616例非糖尿病非裔美国人中空腹胰岛素的定量特征位点。探索了按种族,中枢和年龄调整的按性别分层的线性回归模型。哺乳动物基因分型服务系统输入了391个微卫星标记,间隔约9 cM。使用种族特异性标记等位基因频率和在MERLIN中计算的多点IBD在SOLAR中进行方差分量连锁分析。我们在95 cM(在GATA69E12和GATA71G04之间)的2号染色体上检测到了影响女性受试者空腹胰岛素的定量性状基因座(赔率对数[LOD] = 3.4),但在男性受试者中没有检测到(QD = 0.0,相互作用P = 0.007) 。在欧美(LOD = 2.1)和非裔美国人(LOD = 1.2)女性受试者中均检测到2p13.2的性别特异性信号。我们的发现与胰岛素相关性状的其他几种连锁报道相重叠,并证明了在寻找胰岛素相关基因时考虑复杂的背景相关相互作用的重要性。

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