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Polymorphisms in the Insulin-Degrading Enzyme Gene Are Associated With Type 2 Diabetes in Men From the NHLBI Framingham Heart Study

机译:NHLBI Framingham心脏研究显示,胰岛素降解酶基因的多态性与男性2型糖尿病有关。

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Linkage studies have mapped a susceptibility gene for type 2 diabetes to the long arm of chromosome 10, where we have previously identified a quantitative trait locus that affects fasting blood glucose within the Framingham Heart Study cohort. One candidate gene in this region is the insulin-degrading enzyme (IDE), which, in the GK rat model, has been associated with nonobese type 2 diabetes. Single nucleotide polymorphisms (SNPs) were used to map a haplotype block in the 3′ end of IDE, which revealed association with HbA_(1c), fasting plasma glucose (FPG), and mean fasting plasma glucose (mFPG) measured over 20 years. The strongest associations were found in a sample of unrelated men. The lowest trait values were associated with a haplotype (TT, f~0.32) containing the minor allele of rs2209772 and the major allele of the rs1887922 SNP (FPG P < 0.001, mFPG P < 0.003, HbA_(1c) P < 0.025). Another haplotype (CC, f~0.16) was associated with elevated HbA_(1c) (P < 0.002) and type 2 diabetes (P < 0.001, odds ratio 1.96, 95% CI 1.28-3.00). The evidence presented supports the possibility that IDE is a susceptibility gene for diabetes in populations of European descent.
机译:连锁研究已经将2型糖尿病的易感基因定位在10号染色体的长臂上,我们先前已经确定了一个定量性状基因座,该基因座会影响Framingham心脏研究队列中的空腹血糖。该区域的一个候选基因是胰岛素降解酶(IDE),在GK大鼠模型中,该酶已与非肥胖2型糖尿病相关。单核苷酸多态性(SNPs)用于在IDE的3'端绘制单倍型图谱,这揭示了与HbA_(1c),空腹血糖(FPG)和平均空腹血糖(mFPG)超过20年的关联。在不相关的男性样本中发现最强的关联。最低的性状值与包含rs2209772的次要等位基因和rs1887922 SNP的主要等位基因的单倍型(TT,f〜0.32)相关(FPG P <0.001,mFPG P <0.003,HbA_(1c)P <0.025)。另一单倍型(CC,f〜0.16)与HbA_(1c)升高(P <0.002)和2型糖尿病(P <0.001,优势比1.96,95%CI 1.28-3.00)有关。所提供的证据支持IDE是欧洲血统人群中糖尿病易感基因的可能性。

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