促肾上腺皮质激素释放因子受体亚型1在应激相关功能性结肠改变中的作用:肠易激综合征的意义

Yvette Taché, Vicente Martinez, Mulugeta Million, Celine Maillot
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引用次数: 0

摘要

促肾上腺皮质激素释放因子(CRF)系统的各种元素的鉴定,包括四种哺乳动物CRF相关肽的表征,两种CRF受体亚型1和2 (CRF1)的克隆;CRF2)和选择性CRF1受体拮抗剂的发展使研究人员能够确定CRF信号通路在协调应激反应的生理和行为成分中的重要作用。特别是,令人信服的临床前证据表明,中枢和外周注射CRF都模拟了应激诱导的结肠运动、转运、排便和腹泻的发生,同时肥大细胞脱颗粒,前列腺素E2、粘液和离子渗透性的分泌增加。中枢性CRF还增加了大鼠结肠膨胀引起的腹痛,而外周性CRF降低了人类结肠膨胀引起的痛阈并增加了结肠运动。受体1和2的非选择性CRF拮抗剂和选择性CRF拮抗剂抑制外源性(中枢或外周)CRF,以及急性应激诱导的结肠运动和分泌功能刺激和内脏痛觉过敏。在一项II期临床试验中,CRF1受体介导啮齿动物应激相关的焦虑和抑郁样行为,CRF拮抗剂可减少抑郁。这些发现支持了CRF1受体过度激活可能导致焦虑、抑郁和肠易激综合征合并症的假设。用选择性CRF1拮抗剂靶向这些途径可能是腹泻为主的IBS患者的一种新的治疗途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Role of corticotropin releasing factor receptor subtype 1 in stress-related functional colonic alterations: implications in irritable bowel syndrome.

The identification of the various elements of the Corticotropin Releasing Factor (CRF) system including the characterisation of four mammalian CRF-related peptides, the cloning of two CRF receptor subtypes 1 and 2 (CRF1; CRF2) and the development of selective CRF1 receptor antagonists has allowed investigators to establish an important role for the CRF signalling pathways in coordinating the physiological and behavioural components of the stress response. In particular, compelling preclinical evidence showed that both central and peripheral injection of CRF mimicked stress-induced stimulation of colonic motility, transit, defaecation, and occurrence of diarrhoea along with degranulation of mast cells, and increased secretion of prostaglandin E2, mucus, and ionic permeability. Central CRF also increased abdominal pain from colorectal distention in rats and peripheral CRF reduced pain threshold to colonic distention and increased colonic motility in humans. Non-selective CRF antagonists for receptors 1 and 2 and selective CRF, antagonists inhibit exogenous (central or peripheral) CRF, and acute stress-induced stimulation of colonic motor and secretory function and visceral hyperalgesia. CRF1 receptors mediate stress-related anxiogenic and depression-like behaviours in rodents and CRF, antagonist reduced depression in a phase II clinical trial. These findings lend support to the hypothesis that hyperactivation of CRF1 receptors may contribute to the co-morbidity of anxiety and depression and irritable bowel syndrome. Targeting these pathways with selective CRF1 antagonists may be a novel therapeutic venue for diarrhoea-predominant IBS patients.

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