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早期用于治疗膀胱功能障碍的药物开发——作用于 TRP 通道的药物有希望吗?

Agents in early development for treatment of bladder dysfunction - promise of drugs acting at TRP channels?

机构信息

Institute for Regenerative Medicine, Wake Forest University School of Medicine , Winston Salem , NC , USA.

Institute of Laboratory Medicine, Lund University , Lund , Sweden.

出版信息

Expert Opin Investig Drugs. 2019 Sep;28(9):749-755. doi: 10.1080/13543784.2019.1654994. Epub 2019 Aug 14.

Abstract

: In the lower urinary tract (LUT) several members of the TRP superfamily are involved in nociception and mechanosensory transduction. Animal studies have suggested a therapeutic potential of some of these channels, including TRPV1, TRPV4, TRPM8, TRPA1, and TRPM4, for treatment of bladder over- and underactivity and bladder pain disorders, but translation of this information to clinical application has been slow. : An update on and discussion of current information on the potential clinical use of TRP channel agonists/antagonists in the treatment of different types of bladder dysfunction. The electronic databases PubMed and Scopus were used to identify relevant clinical and animal studies. : The therapeutic effect of TRPV1 channel desensitizing agonists (capsaicin, resiniferatoxin, given intravesically) has been convincingly demonstrated in some forms of bladder overactivity. However, so far, the potential of any of the small-molecule TRP channel blockers developed for non-bladder indications and tested in early human trials for safety has not been explored clinically in LUT dysfunction. The adverse effects of hyperthermia and reduction of noxious heat sensation of the first generation TRPV1 blockers have delayed development. Despite lack of translational information, TRP channels remain interesting targets for future LUT drugs.

摘要

在下尿路 (LUT) 中,TRP 超家族的几个成员参与疼痛和机械感觉转导。动物研究表明,这些通道中的一些具有治疗潜力,包括 TRPV1、TRPV4、TRPM8、TRPA1 和 TRPM4,可用于治疗膀胱过度活动症和膀胱疼痛障碍,但将这些信息转化为临床应用的进展缓慢。

本文更新并讨论了 TRP 通道激动剂/拮抗剂在治疗不同类型膀胱功能障碍中的潜在临床应用的最新信息。使用电子数据库 PubMed 和 Scopus 来确定相关的临床和动物研究。

TRPV1 通道脱敏激动剂(局部给予辣椒素、树脂毒素)已在某些形式的膀胱过度活动症中得到了令人信服的疗效证明。然而,到目前为止,任何为非膀胱适应症开发的小分子 TRP 通道阻滞剂,在早期人体试验中测试其安全性,都尚未在 LUT 功能障碍的临床实践中得到探索。第一代 TRPV1 阻滞剂的高热副作用和有害热感觉的减少延迟了其发展。尽管缺乏转化信息,但 TRP 通道仍然是未来 LUT 药物的有趣靶点。

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