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Chemerin: a potential endocrine link between obesity and type 2 diabetes

机译:Chemerin:肥胖与2型糖尿病之间的潜在内分泌联系

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Obesity and type 2 diabetes have reached epidemic levels and account for a substantial portion of the annual health expenditures of developed nations. While there is an abundance of epidemiological evidence demonstrating that obesity is a primary risk factor for developing type 2 diabetes, the mechanism(s) underlying this linkage are not completely understood. Given the enormous impact of these disorders on global health, considerable research effort has been devoted to elucidate the pathophysiological relationship between these two disorders. Two factors believed to contribute to the causal link between obesity and type 2 diabetes are chronic inflammation and altered secretion of adipose-derived signaling molecules (adipokines). Independent lines of investigation have implicated the novel adipokine chemerin as a regulator of adipogenesis, inflammation, and glucose metabolism through interactions with the cognate cell surface receptor chemokine-like receptor 1. Increased levels of chemerin that occur with obesity are hypothesized to be a causal factor in the development of type 2 diabetes as a consequence of dysregulation of the key physiological processes regulated by this adipokine. This review summarizes current research on the biological roles of chemerin and chemokine-like receptor 1, and highlights key questions to guide future research on the role of this adipokine in mediating obesity and the development of type 2 diabetes.
机译:肥胖和2型糖尿病已达到流行病水平,并占发达国家年度卫生支出的很大一部分。尽管有大量的流行病学证据表明肥胖是发展2型糖尿病的主要危险因素,但这种联系的潜在机制尚不完全清楚。鉴于这些疾病对全球健康的巨大影响,已投入大量研究工作来阐明这两种疾病之间的病理生理关系。认为导致肥胖与2型糖尿病之间存在因果关系的两个因素是慢性炎症和脂肪来源的信号分子(adipokines)分泌的改变。独立研究表明,新的脂肪因子凯莫瑞通过与同源细胞表面受体趋化因子样受体1相互作用,作为脂肪形成,炎症和葡萄糖代谢的调节剂。肥胖引起的凯莫瑞水平升高被认为是一个致病因素由于该脂肪因子调节的关键生理过程失调,导致2型糖尿病的发展。这篇综述总结了关于chemerin和趋化因子样受体1的生物学作用的最新研究,并着重指出了关键问题,以指导有关该脂肪因子在介导肥胖和2型糖尿病发展中作用的未来研究。

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