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黑皮质素4受体(MC4R)和脂肪量和肥胖相关基因(FTO)常见基因变异对欧洲普通人群肥胖的联合影响。

Combined effects of MC4R and FTO common genetic variants on obesity in European general populations.

作者信息

Cauchi Stéphane, Stutzmann Fanny, Cavalcanti-Proença Christine, Durand Emmanuelle, Pouta Anneli, Hartikainen Anna-Liisa, Marre Michel, Vol Sylviane, Tammelin Tuija, Laitinen Jaana, Gonzalez-Izquierdo Arturo, Blakemore Alexandra I F, Elliott Paul, Meyre David, Balkau Beverley, Järvelin Marjo-Riitta, Froguel Philippe

机构信息

CNRS 8090-Institute of Biology, Pasteur Institute, Lille, France.

出版信息

J Mol Med (Berl). 2009 May;87(5):537-46. doi: 10.1007/s00109-009-0451-6. Epub 2009 Mar 3.

Abstract

Genome-wide association scans recently identified common polymorphisms, in intron 1 of FTO and 188 kb downstream MC4R, that modulate body mass index (BMI) and associate with increased risk of obesity. Although their individual contribution to obesity phenotype is modest, their combined effects and their interactions with environmental factors remained to be evaluated in large general populations from birth to adulthood. In the present study, we analyzed independent and combined effects of the FTO rs1421085 and MC4R rs17782313 risk alleles on BMI, fat mass, prevalence and incidence of obesity and subsequent type 2 diabetes (T2D) as well as their interactions with physical activity levels and gender in two European prospective population-based cohorts of 4,762 Finnish adolescents (NFBC 1986) and 3,167 French adults (D.E.S.I.R.). Compared to participants carrying neither FTO nor MC4R risk allele (20-24% of the populations), subjects with three or four risk alleles (7-10% of the populations) had a 3-fold increased susceptibility of developing obesity during childhood. In adults, their combined effects were more modest (approximately 1.8-fold increased risk) and associated with a 1.27% increase in fat mass (P = 0.001). Prospectively, we demonstrated that each FTO and MC4R risk allele increased obesity and T2D incidences by 24% (P = 0.02) and 21% (P = 0.02), respectively. However, the effect on T2D disappeared after adjustment for BMI. The Z-BMI and ponderal index of newborns homozygous for the rs1421085 C allele were 0.1 units (P = 0.02) and 0.27 g/cm(3) (P = 0.005) higher, respectively, than in those without FTO risk allele. The MC4R rs17782313 C allele was more associated with obesity and fat mass deposition in males than in females (P = 0.003 and P = 0.03, respectively) and low physical activity accentuated the effect of the FTO polymorphism on BMI increase and obesity prevalence (P = 0.008 and P = 0.01, respectively). In European general populations, the combined effects of common polymorphisms in FTO and MC4R are therefore additive, predictive of obesity and T2D, and may be influenced by interactions with physical activity levels and gender, respectively.

摘要

全基因组关联扫描最近在FTO基因内含子1以及下游188 kb处的MC4R基因中发现了常见的多态性,这些多态性可调节体重指数(BMI)并与肥胖风险增加相关。尽管它们对肥胖表型的个体贡献不大,但它们的综合作用以及它们与环境因素的相互作用仍有待在从出生到成年的大型普通人群中进行评估。在本研究中,我们分析了FTO基因rs1421085和MC4R基因rs17782313风险等位基因对BMI、脂肪量、肥胖患病率和发病率以及随后的2型糖尿病(T2D)的独立和联合作用,以及它们在两个基于欧洲前瞻性人群的队列中的相互作用,这两个队列分别是4762名芬兰青少年(NFBC 1986)和3167名法国成年人(D.E.S.I.R.),涉及身体活动水平和性别。与既不携带FTO也不携带MC-4R风险等位基因的参与者(占人群的20%-24%)相比,携带三个或四个风险等位基因的受试者(占人群的7%-10%)在儿童期患肥胖症的易感性增加了3倍。在成年人中,它们的联合作用更为适度(风险增加约1.8倍),并与脂肪量增加1.27%相关(P = 0.001)。前瞻性研究表明,每个FTO和MC4R风险等位基因分别使肥胖症和T2D的发病率增加24%(P = 0.02)和21%(P = 0.02)。然而,在调整BMI后,对T2D的影响消失。rs1421085 C等位基因纯合的新生儿的Z-BMI和 ponderal指数分别比没有FTO风险等位基因的新生儿高0.1个单位(P = 0.02)和0.27 g/cm³(P = 0.005)。MC4R rs17782313 C等位基因与男性肥胖和脂肪量沉积的相关性高于女性(分别为P = 0.003和P = 0.03),低身体活动加剧了FTO基因多态性对BMI增加和肥胖患病率的影响(分别为P = 0.008和P = 0.01)。因此,在欧洲普通人群中,FTO和MC4R基因常见多态性的联合作用具有累加性,可预测肥胖症和T2D,并且可能分别受到与身体活动水平和性别的相互作用的影响。

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