韩国人群中reg1α基因多态性与早发性2型糖尿病的关系

Korean diabetes journal Pub Date : 2010-08-01 Epub Date: 2010-08-31 DOI:10.4093/kdj.2010.34.4.229
Bo Kyung Koo, Young Min Cho, Kuchan Kimm, Jong-Young Lee, Bermseok Oh, Byung Lae Park, Hyun Sub Cheong, Hyoung Doo Shin, Kyung Soo Ko, Sang Gyu Park, Hong Kyu Lee, Kyong Soo Park
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引用次数: 2

摘要

背景:据报道,regg基因在再生胰岛中表达,Reg1蛋白在小鼠糖尿病的早期阶段上调。由于人类Reg1α与小鼠Reg1是同源的,我们研究了韩国人群中Reg1α的常见变异是否与2型糖尿病有关。方法:利用24份韩国人DNA样本对Reg1α基因进行测序,以确定常见多态性。在752例2型糖尿病患者和642例非糖尿病患者中,共发现5个多态性(G .- 385t >C [rs10165462]、G .- 36t >G [rs25689789]、G . 209g >T [rs2070707]、G . 1385c >G [novel]和G . 2199g >A [novel])。结果:多态性与2型糖尿病风险无相关性。然而,g.-385C和g.2199A降低了早发性2型糖尿病的风险,早发性2型糖尿病定义为诊断年龄在25岁及以上但小于40岁的受试者(g.-385C和g.2199A的比值比分别为0.721[0.535 ~ 0.971]和0.731 [0.546 ~ 0.977]),g.1385G增加了早发性糖尿病的风险(or为1.398[1.055 ~ 1.854])。虽然对多重假设检验的误差进行校正后发现,三种个体多态性与早发性糖尿病之间没有统计学意义上的关联,但由g.-385C、g.1385C和g.2199A组成的单倍型H1与早发性糖尿病风险降低相关(OR为0.590 [0.396 ~ 0.877],P = 0.009)。结论:Reg1α基因多态性未发现与2型糖尿病的总体易感性相关,尽管在韩国人群中,一些基因多态性与早发性2型糖尿病有一定关联。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Polymorphisms of the reg1α gene and early onset type 2 diabetes in the korean population.

Polymorphisms of the reg1α gene and early onset type 2 diabetes in the korean population.

Polymorphisms of the reg1α gene and early onset type 2 diabetes in the korean population.

Polymorphisms of the reg1α gene and early onset type 2 diabetes in the korean population.

Background: The Reg gene has been reported to be expressed in regenerating islets and Reg1 protein to be up-regulated at an early stage of diabetes in mice. As human Reg1α is homologous with murine Reg1, we investigated whether common variants in Reg1α are associated with type 2 diabetes in the Korean population.

Methods: We sequenced the Reg1α gene to identify common polymorphisms using 24 Korean DNA samples. Of 11 polymorphisms found, five common ones (g.-385T>C [rs10165462], g.-36T>G [rs25689789], g.209G>T [rs2070707], g.1385C>G [novel], and g.2199G>A [novel]) were genotyped in 752 type 2 diabetic patients and 642 non-diabetic subjects.

Results: No polymorphism was associated with the risk of type 2 diabetes. However, g.-385C and g.2199A lowered the risk of early-onset type 2 diabetes, defined as a diagnosis in subjects whose age at diagnosis was 25 years or more but less than 40 years (odds ratio [OR], 0.721 [0.535 to 0.971] and 0.731 [0.546 to 0.977] for g.-385C and g.2199A, respectively) and g.1385G increased the risk of early-onset diabetes (OR, 1.398 [1.055 to 1.854]). Although adjusting for errors in multiple hypotheses-testing showed no statistically significant association between the three individual polymorphisms and early-onset diabetes, the haplotype H1, composed of g.-385C, g.1385C, and g.2199A, was associated with a reduced risk of early-onset diabetes (OR, 0.590 [0.396 to 0.877], P = 0.009).

Conclusion: Polymorphisms in the Reg1α were not found to be associated with overall susceptibility to type 2 diabetes, though some showed modest associations with early-onset type 2 diabetes in the Korean population.

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