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分析骨钙素作为 2 型糖尿病(T2D)及白种人和非裔美国人中间表型的候选基因。

Analysis of osteocalcin as a candidate gene for type 2 diabetes (T2D) and intermediate traits in Caucasians and African Americans.

机构信息

Department of Internal Medicine, Wake Forest University Health Sciences, Winston-Salem, NC, USA.

出版信息

Dis Markers. 2010;28(5):281-6. doi: 10.3233/DMA-2010-0701.

Abstract

Recent studies in mice and human identified osteocalcin (OCN) as a bone-derived hormone that modulates insulin secretion and insulin sensitivity. OCN is synthesized by the bone gamma-carboxyglutamate protein (BGLAP) gene located in the well replicated region of type 2 diabetes (T2D) linkage on chromosome 1q22. We resequenced BGLAP gene in 192 individuals with T2D and performed case-control studies in 766 Caucasian (461 T2D and 305 controls) and 563 African American individuals (371 T2D and 192 controls). Metabolic effects of BGLAP variants were examined in 127 nondiabetic members of Caucasian T2D families and in 498 unrelated nondiabetic African American and Caucasian individuals. BGLAP expression was tested in transformed lymphocytes from 60 Caucasian individuals. We identified 17 single nucleotide polymorphisms (SNPs) in African Americans, but observed only the two known SNPs in Caucasians. No SNP was associated with T2D. Promoter SNP rs1800247 was not associated with metabolic traits including insulin sensitivity (S(I)) or fasting glucose in either population, but nonsynonymous SNP rs34702397 (R94Q) was nominally associated with S(I) (uncorrected p=0.05) and glucose-mediated glucose disposal (S(G); uncorrected p=0.03) in African Americans. No SNP altered measures of insulin secretion or obesity, nor was BGLAP expression associated with rs1800247. Our study was sufficiently powered to exclude BGLAP variants as a major risk factor (OR > 1.5) for T2D in Caucasians, but coding variants in exon 4 may alter glucose homeostasis and diabetes risk in African Americans.

摘要

最近在小鼠和人类中的研究表明,骨钙素(OCN)是一种由骨骼产生的激素,可以调节胰岛素分泌和胰岛素敏感性。OCN 由骨 γ-羧基谷氨酸蛋白(BGLAP)基因合成,该基因位于染色体 1q22 上的 2 型糖尿病(T2D)连锁的高度复制区域。我们对 192 名 T2D 患者的 BGLAP 基因进行了重测序,并在 766 名白种人(461 名 T2D 和 305 名对照)和 563 名非裔美国人个体(371 名 T2D 和 192 名对照)中进行了病例对照研究。在 127 名非糖尿病的白种人 T2D 家族成员和 498 名无关的非裔美国人和白种人中,检测了 BGLAP 变异体的代谢效应。在 60 名白种人个体的转化淋巴细胞中检测了 BGLAP 表达。我们在非裔美国人中发现了 17 个单核苷酸多态性(SNP),但在白种人中只观察到两个已知的 SNP。没有 SNP 与 T2D 相关。启动子 SNP rs1800247 与代谢特征(包括胰岛素敏感性(S(I))或空腹血糖)在两个群体中均无关联,但非同义 SNP rs34702397(R94Q)在非裔美国人中与 S(I)(未经校正的 p=0.05)和葡萄糖介导的葡萄糖处置(S(G);未经校正的 p=0.03)呈名义相关。没有 SNP 改变胰岛素分泌或肥胖的测量值,BGLAP 表达也与 rs1800247 无关。我们的研究有足够的效力排除 BGLAP 变异体作为白种人 T2D 的主要危险因素(OR>1.5),但外显子 4 中的编码变异可能改变非裔美国人的葡萄糖稳态和糖尿病风险。

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