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辣椒素通过 TRPV1 的治疗靶向作用:从临床前研究到临床试验。

Therapeutic targeting of TRPV1 by resiniferatoxin, from preclinical studies to clinical trials.

机构信息

Department of Anesthesiology, Perioperative and Pain Medicine, Brigham and Women's Hospital, Harvard Medical School, Boston, MA 02115, USA.

出版信息

Curr Top Med Chem. 2011;11(17):2159-70. doi: 10.2174/156802611796904924.

DOI:10.2174/156802611796904924
PMID:21671878
Abstract

In primary sensory neurons, the capsaicin receptor TRPV1 functions as a molecular integrator for a broad range of seemingly unrelated chemical and physical noxious stimuli, including heat and altered pH. Indeed, TRPV1 is thought to be a major transducer of the thermal hyperalgesia that follows inflammation and tissue injury as this response is impaired in TRPV1-deficient mice. Following the molecular cloning of TRPV1 in 1997, over a dozen companies embarked on efforts to find clinically useful TRPV1 antagonists, but side-effects and limited efficacy have thus far prevented any compounds from progressing beyond phase II. This has rekindled interest in desensitization of nociceptive neurons to TRPV1 agonists (e.g. capsaicin and its ultrapotent analog resiniferatoxin) as an alternative pharmacological approach to block pain in the periphery where it is generated. The clinical value of capsaicin is, however, limited by its unfavorable irritancy to desensitization ratio. In animal experiments, resiniferatoxin treatment is a powerful approach to achieve long-lasting analgesia. In patients with overactive bladder, intravesical resiniferatoxin improves bladder function (or even restores continence) without significant irritancy and/or toxicity. In this review, we argue that resiniferatoxin is an attractive alternative to capsaicin in that it achieves lasting desensitization without the side effects that complicate capsaicin therapy.

摘要

在初级感觉神经元中,辣椒素受体 TRPV1 作为一种分子整合器,整合了广泛的看似不相关的化学和物理有害刺激,包括热和 pH 值改变。事实上,TRPV1 被认为是炎症和组织损伤后热痛觉过敏的主要转导器,因为 TRPV1 缺陷小鼠的这种反应受损。1997 年 TRPV1 的分子克隆后,有十多家公司开始努力寻找临床上有用的 TRPV1 拮抗剂,但迄今为止,由于副作用和有限的疗效,任何化合物都未能进入二期临床试验。这重新激发了人们对伤害感受神经元脱敏以 TRPV1 激动剂(如辣椒素及其超强效类似物树脂毒素)的兴趣,作为阻断外周疼痛的替代药理学方法,而疼痛是在外周产生的。然而,辣椒素的临床价值受到其脱敏比不理想的刺激性的限制。在动物实验中,树脂毒素治疗是实现长期镇痛的有力方法。在膀胱过度活动症患者中,膀胱内应用树脂毒素可改善膀胱功能(甚至恢复控尿),而无明显的刺激性和/或毒性。在这篇综述中,我们认为,与辣椒素相比,树脂毒素是一种有吸引力的替代品,因为它能实现持久的脱敏,而不会产生使辣椒素治疗复杂化的副作用。

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