辣椒素及其类似物在妇科癌症中的抗癌活性。

Advances in cancer research Pub Date : 2024-01-01 Epub Date: 2024-05-31 DOI:10.1016/bs.acr.2024.05.005
Kathleen C Brown, Amanda M Sugrue, Kaitlyn B Conley, Kushal J Modi, Reagan S Light, Ashley J Cox, Christopher R Bender, Sarah L Miles, Krista L Denning, Paul T Finch, Joshua A Hess, Maria T Tirona, Monica A Valentovic, Piyali Dasgupta
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引用次数: 0

摘要

辣椒素是辣椒中辛辣刺激的成分。它是一种强效镇痛剂,经常用于非处方镇痛乳液和药膏中。多项研究表明,辣椒素在体外和体内对人类癌症具有抑制生长的作用。除了具有抑制生长的活性(作为一种单体制剂)外,还发现辣椒素能使人类癌细胞对化疗和放疗的促凋亡作用敏感。本书第一章讨论了辣椒素在妇科癌症细胞培养实验和小鼠模型中的抗癌活性。在所有妇科癌症中,只有宫颈癌和卵巢癌研究了辣椒素(及其类似物)的抗癌活性。由于辣椒素的生物利用度和水溶性较差,将其作为一种可行的抗癌药物进行临床开发仍具有挑战性。此外,服用辣椒素还伴有胃肠痉挛、胃痛、肠道刺激、恶心、腹泻和呕吐等不良副作用。为了克服辣椒素的这些缺点,人们研究了两种策略。第一种是将辣椒素封装在缓释给药系统中。第二种策略是设计无刺激性的辣椒素类似物,以保留辣椒素的抗肿瘤活性。本章第二部分概述了辣椒素类似物和基于辣椒素的缓释制剂在宫颈癌和卵巢癌中的抗肿瘤(和化疗致敏活性)作用。选择性非刺激性辣椒素类似物和辣椒素基聚合物给药系统的设计可能会为治疗和管理妇科癌症的新策略带来希望。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Anti-cancer activity of capsaicin and its analogs in gynecological cancers.

Capsaicin is the hot and pungent ingredient of chili peppers. It is a potent pain-relieving agent and is often present in over-the-counter analgesic lotions and creams. Several convergent studies reveal that capsaicin displays growth-suppressive activity in human cancers in vitro and in vivo. Apart from its growth-suppressive activity (as a single agent), capsaicin has been found to sensitize human cancer cells to the pro-apoptotic effects of chemotherapy and radiation. The first part of this book chapter discusses the anti-cancer activity of capsaicin in gynecological cancers in cell culture experiments and mouse models. Out of all gynecological cancers, the anti-cancer activity of capsaicin (and its analogs) has only been investigated in cervical cancers and ovarian cancers. The clinical development of capsaicin as a viable anti-cancer drug has remained challenging due to its poor bioavailability and aqueous solubility properties. In addition, the administration of capsaicin is associated with adverse side effects like gastrointestinal cramps, stomach pain, irritation in the gut, nausea diarrhea and vomiting. Two strategies have been investigated to overcome these drawbacks of capsaicin. The first is to encapsulate capsaicin in sustained release drug delivery systems. The second strategy is to design non-pungent capsaicin analogs which will retain the anti-tumor activity of capsaicin. The second part of this chapter provides an overview of the anti-neoplastic (and chemosensitization activity) of capsaicin analogs and capsaicin-based sustained release formulations in cervical and ovarian cancers. The design of selective non-pungent capsaicin analogs and capsaicin-based polymeric drug delivery systems may foster the hope of novel strategies for the treatment and management of gynecological cancers.

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