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首页> 外文期刊>Human Genomics >New susceptibility locus for obesity and dyslipidaemia on chromosome 3q22.3
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New susceptibility locus for obesity and dyslipidaemia on chromosome 3q22.3

机译:3q22.3号染色体上肥胖和血脂异常的新易感性基因座

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Background The muscle Ras ( MRAS ) gene resides on chromosome 3q22.3 and encodes a member of the membrane-associated Ras small GTPase proteins, which function as signal transducers in multiple processes including cell growth and differentiation. Its role in cardiovascular disease is not fully understood yet. In a preliminary study in heterozygous familial hypercholesterolaemia, we identified a locus linking the early onset of coronary artery disease (CAD) to chromosome 3q.22 and elected to sequence the MRAS gene using the MegaBACE DNA analysis system. In the present study, we investigated the association of seven single-nucleotide polymorphisms ( SNPs ) at this locus with CAD and its dyslipidaemia-related risk traits in 4,650 Saudi angiographed individuals using TaqMan assays by the Applied Biosystems real-time Prism 7900HT Sequence Detection System. Results Among the studied SNPs , rs6782181 ( p = 0.017) and rs9818870T ( p = 0.009) were associated with CAD following adjustment for sex, age and other confounding risk factors. The rs6782181_GG also conferred risk for obesity (1,764 cases vs. 2,586 controls) [1.16(1.03–1.30); p = 0.017], hypercholesterolaemia (1,686 vs. 2,744) [1.23(1.02–1.47); p = 0.019], hypertriglyceridaemia (1,155 vs. 3,496) [1.29(1.01–1.45); p = 0.043] and low high-density lipoprotein-cholesterol (lHDL-chol) levels (1,935 vs. 2,401) [1.15(1.02–1.30); p = 0.023] after adjustment. Additionally, rs253662_(CT+TT) [1.16(1.01–1.32); p = 0.030] was associated with lHDL-chol levels. Interestingly, rs253662 ( p = 0.014) and rs6782181 ( p = 0.019) were protective against acquiring high low-density lipoprotein-cholesterol (hLDL-chol) levels ( p = 0.014), while rs1720819 showed similar effects against CAD ( p χ 2 = 7.66; p = 0.0056), constructed from the studied SNPs , its 6-mer derivative CCTGAC ( χ 2 = 6.90; p = 0.0086) and several other shorter derivatives conferred risk for obesity. hLDL-chol was weakly linked to CTAA ( χ 2 = 3.79; p = 0.052) and CCT ( χ 2 = 4.32; p = 0.038), while several other haplotypes were protective against both obesity and hLDL-chol level. Conclusion Our results demonstrate that the genomic locus for the MRAS gene confers risk for CAD, obesity and dyslipidaemia and point to the possible involvement of other genes or regulatory elements at this locus, rather than changes in the M-Ras protein function, in these events.
机译:背景肌肉Ras(MRAS)基因位于3q22.3染色体上,编码与膜相关的Ras小GTPase蛋白的成员,该蛋白在包括细胞生长和分化在内的多个过程中充当信号转导者。尚未完全了解其在心血管疾病中的作用。在杂合性家族性高胆固醇血症的一项初步研究中,我们确定了一个将冠状动脉疾病(CAD)的早期发作与染色体3q.22相关联的基因座,并选择使用MegaBACE DNA分析系统对MRAS基因进行测序。在本研究中,我们使用Applied Biosystems实时Prism 7900HT序列检测系统进行TaqMan分析,调查了4,650位沙特血管造影个体中该位点的7个单核苷酸多态性(SNP)与CAD及其与血脂异常相关的危险性状的关联。 。结果在对性别,年龄和其他混杂危险因素进行调整后,研究的SNP中rs6782181(p = 0.017)和rs9818870T(p = 0.009)与CAD相关。 rs6782181_GG还赋予了肥胖风险(1,764例vs. 2,586例对照)[1.16(1.03-1.30); p = 0.017],高胆固醇血症(1,686 vs. 2,744)[1.23(1.02-1.47); p = 0.019],高甘油三酯血症(1,155 vs. 3,496)[1.29(1.01-1.45); p = 0.043]和低密度脂蛋白胆固醇(lHDL-chol)水平较低(1,935对2,401)[1.15(1.02-1.30); p = 0.023]。此外,rs253662_(CT + TT)[1.16(1.01–1.32); p = 0.030]与1HDL-胆固醇水平相关。有趣的是,rs253662(p = 0.014)和rs6782181(p = 0.019)可以防止获得高低密度脂蛋白胆固醇(hLDL-chol)水平(p = 0.014),而rs1720819也显示出类似的抗CAD作用(pχ 2 = 7.66; p = 0.0056),由研究的SNP及其6-mer衍生物CCTGAC构成(χ 2 = 6.90; p = 0.0086)和其他几种较短的衍生物可能会导致肥胖。 hLDL-chol与CTAA(χ 2 = 3.79; p = 0.052)和CCT(χ 2 = 4.32; p = 0.038),而其他几种单倍型对肥胖和hLDL-chol水平均具有保护作用。结论我们的结果表明,在这些事件中,MRAS基因的基因座可赋予CAD,肥胖和血脂异常的风险,并指出其他基因或调控元件可能参与该基因座,而不是M-Ras蛋白功能的改变。

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