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Cadm2 regulates body weight and energy homeostasis in mice

机译:Cadm2调节小鼠的体重和能量稳态

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Objective Obesity is strongly linked to genes regulating neuronal signaling and function, implicating the central nervous system in the maintenance of body weight and energy metabolism. Genome-wide association studies identified significant associations between body mass index (BMI) and multiple loci near Cell adhesion molecule2 ( CADM2 ), which encodes a mediator of synaptic signaling enriched in the brain. Here we sought to further understand the role of Cadm2 in the pathogenesis of hyperglycemia and weight gain. Methods We first analyzed Cadm2 expression in the brain of both human subjects and mouse models and subsequently characterized a loss-of-function mouse model of Cadm2 for alterations in glucose and energy homeostasis. Results We show that the risk variant rs13078960 associates with increased CADM2 expression in the hypothalamus of human subjects. Increased Cadm2 expression in several brain regions of Lep ob/ob mice was ameliorated after leptin treatment. Deletion of Cadm2 in obese mice (Cadm2/ob) resulted in reduced adiposity, systemic glucose levels, and improved insulin sensitivity. Cadm2 -deficient mice exhibited increased locomotor activity, energy expenditure rate, and core body temperature identifying Cadm2 as a potent regulator of systemic energy homeostasis. Conclusions Together these data illustrate that reducing Cadm2 expression can reverse several traits associated with the metabolic syndrome including obesity, insulin resistance, and impaired glucose homeostasis.
机译:目的肥胖与调节神经元信号传导和功能的基因密切相关,在维持体重和能量代谢方面牵涉中枢神经系统。全基因组关联研究确定了体重指数(BMI)与靠近细胞粘附分子2(CADM2)的多个基因座之间的显着关联,该基因编码富含大脑的突触信号传导的介质。在这里,我们试图进一步了解Cadm2在高血糖和体重增加的发病机理中的作用。方法我们首先分析了人类受试者和小鼠模型的大脑中Cadm2的表达,然后表征了Cadm2功能丧失的小鼠模型中葡萄糖和能量稳态的改变。结果我们显示,风险变异体rs13078960与人类受试者下丘脑中CADM2表达的增加有关。瘦素治疗后,Lep ob / ob 小鼠的多个脑区域中Cadm2表达的增加得以改善。肥胖小鼠(Cadm2 / ob)中Cadm2的缺失导致肥胖,全身葡萄糖水平降低和胰岛素敏感性提高。缺乏Cadm2的小鼠表现出运动活动增加,能量消耗率和核心体温升高,这表明Cadm2是系统性能量稳态的有效调节剂。结论这些数据共同表明,降低Cadm2表达可以逆转与代谢综合征相关的多个特征,包括肥胖,胰岛素抵抗和葡萄糖稳态下降。

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