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单变量和双变量连锁分析确定了脂质水平和2型糖尿病风险背后的多效性基因座。

Univariate and bivariate linkage analysis identifies pleiotropic loci underlying lipid levels and type 2 diabetes risk.

作者信息

Hasstedt Sandra J, Hanis Craig L, Elbein Steven C

机构信息

Department of Human Genetics, University of Utah, Salt Lake City, Utah 84112-5330, USA.

出版信息

Ann Hum Genet. 2010 Jul;74(4):308-15. doi: 10.1111/j.1469-1809.2010.00589.x.

Abstract

Dyslipidemia frequently co-occurs with type 2 diabetes (T2D) and with obesity. To investigate whether the co-occurrence is due to pleiotropic genes, we performed univariate linkage analysis of lipid levels and bivariate linkage analysis of pairs of lipid levels and of lipid levels paired with T2D, body mass index (BMI), and waist-hip ratio (WHR) in the African American subset of the Genetics of NIDDM (GENNID) sample. We obtained significant evidence for a pleiotropic low density lipoprotein cholesterol (LDL-C)-T2D locus on chromosome 1 at 16-19 megabases (MB) (bivariate lod = 4.41), as well as a non-pleiotropic triglyceride (TG) locus on chromosome 20 at 28-34 MB (univariate lod = 3.57). In addition, near-significant evidence supported TG-T2D loci on chromosome 2 at 81-101 MB (bivariate lod = 4.23) and 232-239 MB (bivariate lod = 4.27) and on chromosome 7 at 147-151 MB (univariate lod = 3.08 for TG with P = 0.041 supporting pleiotropy with T2D), as well as an LDL-C-BMI locus on chromosome 3 at 137-147 MB (bivariate lod score = 4.25). These findings provide evidence that at least some of the co-occurrence of dyslipidemia with T2D and obesity is due to common underlying genes.

摘要

血脂异常常与2型糖尿病(T2D)及肥胖症同时出现。为了研究这种共现情况是否是由于多效性基因所致,我们在非胰岛素依赖型糖尿病遗传学(GENNID)样本的非裔美国人子集中,对血脂水平进行了单变量连锁分析,并对血脂水平对以及与T2D、体重指数(BMI)和腰臀比(WHR)配对的血脂水平进行了双变量连锁分析。我们获得了显著证据,表明在1号染色体上16 - 19兆碱基(MB)处存在一个多效性低密度脂蛋白胆固醇(LDL - C) - T2D位点(双变量对数优势比 = 4.41),以及在20号染色体上28 - 34 MB处存在一个非多效性甘油三酯(TG)位点(单变量对数优势比 = 3.57)。此外,接近显著的证据支持在2号染色体上81 - 101 MB(双变量对数优势比 = 4.23)和232 - 239 MB(双变量对数优势比 = 4.27)以及7号染色体上147 - 151 MB处的TG - T2D位点(TG的单变量对数优势比 = 3.08,P = 0.041支持与T2D的多效性),以及在3号染色体上137 - 147 MB处的一个LDL - C - BMI位点(双变量对数优势比分数 = 4.25)。这些发现提供了证据,表明血脂异常与T2D和肥胖症的至少部分共现情况是由于共同的潜在基因所致。

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