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在魁北克家族研究和瑞典肥胖受试者队列中,β3肾上腺素能受体基因的色氨酸64精氨酸突变对肥胖表型没有影响。

The Trp64Arg mutation of the beta3 adrenergic receptor gene has no effect on obesity phenotypes in the Québec Family Study and Swedish Obese Subjects cohorts.

作者信息

Gagnon J, Mauriège P, Roy S, Sjöström D, Chagnon Y C, Dionne F T, Oppert J M, Pérusse L, Sjöström L, Bouchard C

机构信息

Physical Activity Sciences Laboratory, Laval University, Québec, Canada.

出版信息

J Clin Invest. 1996 Nov 1;98(9):2086-93. doi: 10.1172/JCI119014.

Abstract

The beta adrenergic system plays a key role in regulating energy balance through the stimulation of both thermogenesis and lipid mobilization in brown and white adipose tissues in human and various animal models. Recent studies have suggested that a missense Trp64Arg mutation in the beta3 adrenergic receptor (ADRB3) gene was involved in obesity and insulin resistance. We have investigated the effect of this mutation on obesity-related phenotypes in two cohorts: the Québec Family Study (QFS) and the Swedish Obese Subjects (SOS). In QFS, no association was found between this mutation and body mass index (BMI), body fat including abdominal visceral fat, resting metabolic rate, various diabetes and cardiovascular risk factors, and changes in body weight and body fat over a 12-yr period. With the exception of RMR (P = 0.04), no evidence of linkage was detected between the mutation and phenotypes of QFS based on sib-pair data. In SOS, the frequency of the Trp64Arg allele was not significantly different between nonobese and obese female subjects and no association was found between the mutation and body weight gain over time. These findings do not support the view that there is an association between the Trp64Arg mutation in the ADRB3 gene and obesity.

摘要

β-肾上腺素能系统在调节能量平衡中发挥关键作用,通过刺激人和各种动物模型的棕色和白色脂肪组织中的产热和脂质动员来实现。最近的研究表明,β3-肾上腺素能受体(ADRB3)基因中的一个错义Trp64Arg突变与肥胖和胰岛素抵抗有关。我们在两个队列中研究了这种突变对肥胖相关表型的影响:魁北克家庭研究(QFS)和瑞典肥胖受试者(SOS)。在QFS中,未发现该突变与体重指数(BMI)、包括腹部内脏脂肪在内的体脂、静息代谢率、各种糖尿病和心血管危险因素以及12年期间体重和体脂变化之间存在关联。除静息代谢率外(P = 0.04),根据同胞对数据,未检测到该突变与QFS表型之间存在连锁证据。在SOS中,非肥胖和肥胖女性受试者之间Trp64Arg等位基因的频率没有显著差异,并且未发现该突变与随时间的体重增加之间存在关联。这些发现不支持ADRB3基因中的Trp64Arg突变与肥胖之间存在关联的观点。

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