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探究促肾上腺皮质激素释放因子受体对进食及胃肠结肠动力的调控作用

Nibbling at CRF receptor control of feeding and gastrocolonic motility.

作者信息

Zorrilla Eric P, Taché Yvette, Koob George F

机构信息

Department of Neuropharmacology, The Scripps Research Institute, 10550 North Torrey Pines Road, La Jolla, CA 92037, USA.

出版信息

Trends Pharmacol Sci. 2003 Aug;24(8):421-7. doi: 10.1016/S0165-6147(03)00177-9.

Abstract

Inadequate pharmacological tools, until recently, hindered the understanding of the roles of corticotropin-releasing factor (CRF) receptor subtypes in appetite regulation and gastrocolonic motor function. Now, novel ligands that are selective for CRF(1) or CRF(2) receptors are helping to uncover the specific functions of CRF receptor subtypes. Central or peripheral CRF(2) receptor activation suppresses feeding independently of CRF(1) receptors. In the rat, central administration of CRF(2) receptor agonists promotes satiation without eliciting the malaise, behavioral arousal or anxiogenesis associated with CRF(1) receptor agonists. Conversely, central administration of CRF(1) receptor agonists elicits short-onset anorexia independently of CRF(2) receptor activation. With respect to gastrointestinal motor function, stress inhibits gastric motility through CRF(2) receptor-dependent central autonomic and peripheral myenteric systems. By contrast, stress stimulates colonic motility via CRF(1) receptor-dependent sacral parasympathetic and colonic myenteric mechanisms. These findings have important physiological implications and suggest targeted approaches for the pharmacotherapy of obesity and stress-related functional gastrointestinal and eating disorders.

摘要

直到最近,药理学工具的不足一直阻碍着人们对促肾上腺皮质激素释放因子(CRF)受体亚型在食欲调节和胃肠结肠运动功能中作用的理解。现在,对CRF(1)或CRF(2)受体具有选择性的新型配体正有助于揭示CRF受体亚型的特定功能。中枢或外周CRF(2)受体激活可独立于CRF(1)受体抑制进食。在大鼠中,中枢给予CRF(2)受体激动剂可促进饱腹感,而不会引发与CRF(1)受体激动剂相关的不适、行为觉醒或焦虑症。相反,中枢给予CRF(1)受体激动剂可独立于CRF(2)受体激活引发短期厌食。关于胃肠运动功能,应激通过CRF(2)受体依赖性中枢自主神经系统和外周肠肌系统抑制胃动力。相比之下,应激通过CRF(1)受体依赖性骶副交感神经和结肠肠肌机制刺激结肠动力。这些发现具有重要的生理学意义,并为肥胖症以及与应激相关的功能性胃肠和饮食失调的药物治疗提出了有针对性的方法。

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