Cauchi Stéphane, Froguel Philippe
Curr Diab Rep. 2008 Apr;8(2):149-55. doi: 10.1007/s11892-008-0026-x.
After two decades of limited success, the genetic architecture of type 2 diabetes (T2D) is finally being revealed. Within only 2 years, an avalanche of studies identified several genes expressed in pancreatic beta cells and involved in the control of insulin secretion, such as transcription factor 7-like 2 (TCF7L2), a key element of the Wnt signaling pathway. In Europeans, genome-wide association scans showed that TCF7L2 has been the most important locus predisposing to T2D so far. For the first time, a gene is consistently involved in T2D susceptibility in all major ethnic groups. At the individual level, carrying the TCF7L2 risk allele increases T2D risk 50%. However, at the population level, the attributable risk is lower than 25% and varies with the allele frequency. The presence of the TCF7L2 rs7903146 risk allele increases TCF7L2 gene expression in beta cells, possibly impairing glucagon-like peptide-1-induced insulin secretion and/or the production of new mature beta cells. The tremendous association of TCF7L2 polymorphisms with T2D provides new insights into future genetic predisposition tests but remains the tip of the T2D genetic iceberg.
在经历了二十年的有限成功之后,2型糖尿病(T2D)的遗传结构终于开始显现。在短短两年内,大量研究发现了几个在胰腺β细胞中表达且参与胰岛素分泌调控的基因,比如转录因子7样2(TCF7L2),它是Wnt信号通路的关键元件。在欧洲人群中,全基因组关联扫描显示,TCF7L2是迄今为止导致T2D的最重要基因位点。首次有一个基因在所有主要种族群体的T2D易感性中都持续发挥作用。在个体层面,携带TCF7L2风险等位基因会使T2D风险增加50%。然而,在人群层面,归因风险低于25%,且会随等位基因频率而变化。TCF7L2 rs7903146风险等位基因的存在会增加β细胞中TCF7L2基因的表达,可能会损害胰高血糖素样肽1诱导的胰岛素分泌和/或新成熟β细胞的产生。TCF7L2多态性与T2D之间的巨大关联为未来的遗传易感性检测提供了新的见解,但这仍然只是T2D遗传冰山的一角。
