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Genetic variants associated with lean and obese type 2 diabetes in a Han Chinese population

机译:汉族人群中与肥胖和肥胖的2型糖尿病相关的遗传变异

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摘要

Type 2 diabetes (T2D) is highly phenotypically heterogeneous. Genetics of the heterogeneity of lean and obese T2D is not clear. The aim of the present study was to identify the associations of T2D-related genetic variants with the risks for lean and obese T2D among the Chinese Han population. A case–control study consisting of 5338 T2D patients and 4663 normal glycemic controls of Chinese Han recruited in the Chinese National Diabetes and Metabolic Disorders Study was conducted. T2D cases were identified according to the 1999 World Health Organization criteria. Lean T2D was defined as T2D patient with a body mass index (BMI) <23 kg/m2, whereas obese T2D was defined as T2D patient with a BMI ≥28 kg/m2. Twenty-five genome-wide association studies previously validated T2D-related single-nucleotide polymorphisms (SNPs) were genotyped. A genotype risk score (GRS) based on the 25 SNPs was created. After adjusting for multiple covariates, SNPs in or near CDKAL1, CDKN2BAS, KCNQ1, TCF7L2, CDC123/CAMK1D, HHEX, and TCF2 were associated with the risk for lean T2D, and SNPs in or near KCNQ1 and FTO were associated with the risk for obese T2D. The results showed that the GRS for 25 T2D-related SNPs was more strongly associated with the risk for lean T2D (Ptrend = 2.66 × 10−12) than for obese T2D (Ptrend = 2.91 × 10−5) in our study population. Notably, the T2D GRS contributed to lower obesity-related measurements and greater β-cell dysfunction, including lower insulin levels in oral glucose tolerance test, decreased insulinogenic index, and Homeostasis Model Assessment for β-cell Function. In conclusion, our findings identified T2D-related genetic loci that contribute to the risk of lean and obese T2D individually and additively in a Chinese Han population. Moreover, the study highlights the contribution of known T2D genomic loci to the heterogeneity of lean and obese T2D in Chinese Hans.
机译:2型糖尿病(T2D)具有高度表型异质性。瘦和肥胖T2D异质性的遗传学尚不清楚。本研究的目的是确定中国汉族人群中与T2D相关的遗传变异与瘦型和肥胖型T2D风险的相关性。进行了一项包括5338名T2D患者和4663名中国汉族正常血糖控制者的病例对照研究,该研究纳入了《中国糖尿病和代谢性疾病研究》。根据1999年世界卫生组织的标准确定了T2D病例。瘦型T2D被定义为体重指数(BMI)<23 kg / m 2 的T2D患者,而肥胖型T2D被定义为BMI≥28kg / m 2 < / sup>。对25个全基因组关联研究进行基因分型,该研究先前已验证T2D相关的单核苷酸多态性(SNP)。创建了基于25个SNP的基因型风险评分(GRS)。在对多个协变量进行调整后,CDKAL1,CDKN2BAS,KCNQ1,TCF7L2,CDC123 / CAMK1D,HHEX和TCF2或其附近的SNP与瘦T2D风险相关,而KCNQ1和FTO或其附近的SNP与肥胖风险相关。 T2D。结果表明,与肥胖T2D(Ptrend = 2.91×10 -12 )的肥胖相比,25个T2D相关SNP的GRS与肥胖T2D风险的相关性更高。 > −5 )。值得注意的是,T2D GRS有助于降低与肥胖相关的测量结果和更大的β细胞功能障碍,包括降低口服葡萄糖耐量试验中的胰岛素水平,降低胰岛素生成指数以及针对β细胞功能的稳态模型评估。总之,我们的发现确定了与T2D相关的基因位点,这些基因位点在中国汉族人群中单独和累加了肥胖和肥胖T2D的风险。此外,该研究突出了已知的T2D基因组基因座对中国汉族人群瘦型和肥胖型T2D异质性的贡献。

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