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Cannabinoids and Gastrointestinal Motility: Pharmacology Clinical Effects and Potential Therapeutics in Humans

机译:大麻素和胃肠动力:人体药理学临床作用和潜在治疗方法

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摘要

The objective of this article is to increase the awareness of gastroenterologists to the effects of cannabinoids on gastrointestinal motility, as gastroenterologists are likely to encounter patients who are taking cannabinoids, or those with dysmotility that may be associated with cannabinoid mechanisms. The non-selective cannabinoid agonist, dronabinol, retards gastric emptying and inhibits colonic tone and phasic pressure activity. In addition to the well-recognized manifestations of cannabinoid hyperemesis, cannabinoid mechanisms result in human and animal models of gastrointestinal and colonic dysmotility. Decreased enteric FAAH activity is associated with colonic inertia in slow transit constipation and, conversely, the orphan G-protein coupled receptor, GPR55, is overexpressed in streptozotocin-induced gastroparesis, suggesting it is involved in inhibition of antral motility. Experimental therapies in gastrointestinal motility and functional disorders are focused predominantly on pain relief mediated through cannabinoid 2 receptors or inhibition of DAGLα to normalize colonic transit. In summary, cannabinoid mechanisms and pharmacology are relevant to the current and future practice of clinical gastroenterology.
机译:本文的目的是提高肠胃科医生对大麻素对胃肠动力的影响的认识,因为肠胃科医生可能会遇到正在服用大麻素或患有可能与大麻素机制有关的运动障碍的患者。非选择性大麻素激动剂Dronabinol可延迟胃排空并抑制结肠张力和相压活动。除了公认的大麻素呕吐表现外,大麻素机制还导致人和动物胃肠道和结肠运动障碍模型的出现。肠道FAAH活性降低与慢行便秘中的结肠惯性有关,相反,孤儿G蛋白偶联受体GPR55在链脲佐菌素诱发的胃轻瘫中过表达,表明它参与了对肛门运动的抑制。胃肠动力和功能障碍的实验疗法主要集中在通过大麻素2受体或抑制DAGLα介导的结肠运输正常化所引起的疼痛缓解上。总之,大麻素的作用机理和药理作用与当前和未来临床胃肠病学的实践有关。

著录项

  • 期刊名称 other
  • 作者

    Michael Camilleri;

  • 作者单位
  • 年(卷),期 -1(30),9
  • 年度 -1
  • 页码 e13370
  • 总页数 19
  • 原文格式 PDF
  • 正文语种
  • 中图分类
  • 关键词

    anandamide 2-AG FAAH DAGL;

    机译:阿南酰胺;2-AG;FAAH;DAGL;

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