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人体棕色脂肪组织作为肥胖管理的靶点:超越冷诱导产热。

Human brown adipose tissue as a target for obesity management; beyond cold-induced thermogenesis.

机构信息

Metabolic and Vascular Physiology Laboratory, Baker Heart and Diabetes Institute, Melbourne, Australia.

出版信息

Obes Rev. 2017 Nov;18(11):1227-1242. doi: 10.1111/obr.12584. Epub 2017 Jul 14.

Abstract

Elevating energy expenditure via adaptive thermogenesis in brown adipose tissue (BAT) is a potential strategy to reverse obesity. Much early enthusiasm for this approach, based on rodent studies, was tempered by the belief that BAT was relatively inconsequential in healthy adult humans. Interest was reinvigorated a decade ago when a series of studies re-identified BAT, primarily in upper thoracic regions, in adults. Despite the ensuing explosion of pre-clinical investigations and identification of an extensive list of potential target molecules for BAT recruitment, our understanding of human BAT physiology remains limited, particularly regarding interventions which might hold therapeutic promise. Cold-induced BAT thermogenesis (CIT) has been well studied, although is not readily translatable as an anti-obesity approach, whereas little is known regarding the role of BAT in human diet-induced thermogenesis (DIT). Furthermore, human studies dedicated to translating known pharmacological mechanisms of adipose browning from animal models are sparse. Several lines of recent evidence suggest that molecular regulation and physiology of human BAT differ to that of laboratory rodents, which form the majority of our knowledge base. This review will summarize knowledge on CIT and expand upon the current understanding and evidence gaps related to human adaptive thermogenesis via mechanisms other than cold.

摘要

通过棕色脂肪组织(BAT)的适应性产热来提高能量消耗是逆转肥胖的一种潜在策略。早期基于啮齿动物研究的这种方法曾引起了很大的兴趣,但由于人们认为 BAT 在健康成年人体内相对不重要,这种兴趣后来有所减弱。十年前,一系列重新鉴定 BAT(主要在上胸部)的研究激起了人们的兴趣。尽管随后进行了大量的临床前研究,并确定了一系列潜在的 BAT 募集靶点分子,但我们对人类 BAT 生理学的理解仍然有限,特别是对于那些可能具有治疗前景的干预措施。冷诱导 BAT 产热(CIT)已得到充分研究,但作为一种抗肥胖方法并不容易转化,而对于 BAT 在人类饮食诱导产热(DIT)中的作用知之甚少。此外,专门从动物模型翻译已知脂肪褐变的药理学机制的人类研究很少。最近有几条证据表明,人类 BAT 的分子调节和生理学与实验室啮齿动物不同,而啮齿动物是我们大部分知识基础的来源。这篇综述将总结 CIT 的知识,并扩展目前对人类适应性产热的理解,除了冷之外,还涉及其他机制。

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