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Insights into the Genetic Susceptibility to Type 2 Diabetes from Genome-Wide Association Studies of Glycaemic Traits

机译:血糖性状的全基因组关联研究对2型糖尿病遗传易感性的洞见

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摘要

Over the past 8 years, the genetics of complex traits have benefited from an unprecedented advancement in the identification of common variant loci for diseases such as type 2 diabetes (T2D). The ability to undertake genome-wide association studies in large population-based samples for quantitative glycaemic traits has permitted us to explore the hypothesis that models arising from studies in non-diabetic individuals may reflect mechanisms involved in the pathogenesis of diabetes. Amongst 88 T2D risk and 72 glycaemic trait loci, only 29 are shared and show disproportionate magnitudes of phenotypic effects. Important mechanistic insights have been gained regarding the physiological role of T2D loci in disease predisposition through the elucidation of their contribution to glycaemic trait variability. Further investigation is warranted to define causal variants within these loci, including functional characterisation of associated variants, to dissect their role in disease mechanisms and to enable clinical translation.
机译:在过去的8年中,复杂性状的遗传学得益于鉴定常见疾病(如2型糖尿病(T2D))变异位点的空前发展。在大量的基于人群的样本中进行定量的血糖特征进行全基因组关联研究的能力使我们能够探索这样一个假设,即非糖尿病个体研究产生的模型可能反映了糖尿病发病机理。在88个T2D风险和72个血糖性状基因座中,只有29个共享并且显示出不均衡的表型效应。通过阐明T2D基因座对血糖性状变异的贡献,已经获得了有关T2D基因座在疾病易感性中的生理作用的重要机制的见解。有必要进行进一步的研究以定义这些基因座内的因果变异,包括相关变异的功能表征,以剖析其在疾病机制中的作用并进行临床翻译。

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