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内脂素基因(PBEF1)启动子区域的常见多态性影响法裔加拿大人群的血浆胰岛素水平。

Common polymorphisms in the promoter of the visfatin gene (PBEF1) influence plasma insulin levels in a French-Canadian population.

作者信息

Bailey Swneke D, Loredo-Osti J C, Lepage Pierre, Faith Janet, Fontaine Joelle, Desbiens Katia M, Hudson Thomas J, Bouchard Claude, Gaudet Daniel, Pérusse Louis, Vohl Marie-Claude, Engert James C

机构信息

Department of Human Genetics, McGill University, Montréal, Québec, Canada H3A 1A1.

出版信息

Diabetes. 2006 Oct;55(10):2896-902. doi: 10.2337/db06-0189.

Abstract

The adipokine visfatin (PBEF1) exhibits insulin-mimetic effects and correlates strongly with visceral adiposity. We sequenced visfatin gene exons and 1,480 bp of the promoter in 23 individuals, including 18 individuals from the Quebec Family Study (QFS) with varying degrees of abdominal visceral fat, assessed by computed tomography, and 5 individuals from the Saguenay-Lac-Saint-Jean region of Québec. We identified a synonymous polymorphism in exon 7 (SER301SER) but no nonsynonymous mutations. We observed an additional 10 polymorphisms, including 5 intronic, 4 within the promoter, and 1 within the 3' untranslated region. Further promoter sequencing (816 bp) identified five additional single nucleotide polymorphisms (SNPs) in the QFS population. To investigate the role of visfatin gene variants in obesity-related phenotypes, we genotyped a total of 13 SNPs in the promoter region of the gene. From these, we analyzed the seven common SNPs in the QFS sample (918 participants from 208 families). A significant association was found between two SNPs (rs9770242 and rs1319501), in perfect linkage disequilibrium, and fasting insulin levels (P = 0.002). These SNPs were also associated with fasting glucose (P <or= 0.02). In addition, a more distal SNP (rs7789066) was significantly associated with the apolipoprotein B component of VLDL (P = 0.012).

摘要

脂肪因子内脂素(PBEF1)具有胰岛素模拟作用,且与内脏肥胖密切相关。我们对23名个体的内脂素基因外显子及1480 bp的启动子进行了测序,其中包括来自魁北克家族研究(QFS)的18名个体,他们通过计算机断层扫描评估具有不同程度的腹部内脏脂肪,以及来自魁北克萨格奈-圣让湖地区的5名个体。我们在第7外显子中鉴定出一个同义多态性(SER301SER),但未发现非同义突变。我们还观察到另外10个多态性,包括5个内含子多态性、4个启动子区域内的多态性以及3'非翻译区内的1个多态性。进一步的启动子测序(816 bp)在QFS人群中又鉴定出另外5个单核苷酸多态性(SNP)。为了研究内脂素基因变异在肥胖相关表型中的作用,我们对该基因启动子区域总共13个SNP进行了基因分型。从中,我们分析了QFS样本(来自208个家庭的918名参与者)中的7个常见SNP。发现两个处于完全连锁不平衡状态的SNP(rs9770242和rs1319501)与空腹胰岛素水平显著相关(P = 0.002)。这些SNP也与空腹血糖相关(P≤0.02)。此外,一个更远端的SNP(rs7789066)与极低密度脂蛋白(VLDL)的载脂蛋白B成分显著相关(P = 0.012)。

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