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走向有效的外周内脏镇痛:应对全国阿片类药物危机。

Toward an effective peripheral visceral analgesic: responding to the national opioid crisis.

机构信息

Clinical Enteric Neuroscience Translational and Epidemiological Research Center, Mayo Clinic , Rochester, Minnesota.

出版信息

Am J Physiol Gastrointest Liver Physiol. 2018 Jun 1;314(6):G637-G646. doi: 10.1152/ajpgi.00013.2018. Epub 2018 Feb 22.

Abstract

This minireiew summarizes recent new developments in visceral analgesics. This promising field is important, as a new approach to address abdominal pain with peripheral visceral analgesics is considered a key approach to addressing the current opioid crisis. Some of the novel compounds address peripheral pain mechanisms through modulation of opioid receptors via biased ligands, nociceptin/orphanin FQ opioid peptide (NOP) receptor, or dual action on NOP and μ-opioid receptor, buprenorphine and morphiceptin analogs. Other compounds target nonopioid mechanisms, including cannabinoid (CB2), N-methyl-d-aspartate, calcitonin gene-related peptide, estrogen, and adenosine A receptors and transient receptor potential (TRP) channels (TRPV1, TRPV4, and TRPM8). Although current evidence is based predominantly on animal models of visceral pain, early human studies also support the evidence from the basic and animal research. This augurs well for the development of nonaddictive, visceral analgesics for treatment of chronic abdominal pain, an unmet clinical need.

摘要

这篇综述总结了内脏镇痛药的最新新进展。这个有前景的领域很重要,因为外周内脏镇痛药的新方法被认为是解决当前阿片类药物危机的关键方法。一些新型化合物通过偏向配体、孤啡肽/孤啡肽 FQ 阿片肽(NOP)受体或双重作用于 NOP 和 μ-阿片受体、丁丙诺啡和吗啡肽类似物来调节阿片受体,从而针对外周疼痛机制。其他化合物针对非阿片类机制,包括大麻素 (CB2)、N-甲基-D-天冬氨酸、降钙素基因相关肽、雌激素和腺苷 A 受体和瞬时受体电位 (TRP) 通道 (TRPV1、TRPV4 和 TRPM8)。尽管目前的证据主要基于内脏疼痛的动物模型,但早期的人类研究也支持基础和动物研究的证据。这为开发用于治疗慢性腹痛的非成瘾性内脏镇痛药带来了良好的前景,这是一种未满足的临床需求。

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