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局部克罗米通、辣椒素和皮质类固醇对瘙痒原诱导的搔抓行为的止痒作用。

Anti pruritic effects of topical crotamiton, capsaicin, and a corticosteroid on pruritogen-induced scratching behavior.

机构信息

Department of Dermatology, Graduate School, Tokyo Medical and Dental University, Tokyo, Japan.

出版信息

Exp Dermatol. 2012 Mar;21(3):201-4. doi: 10.1111/j.1600-0625.2011.01433.x.

DOI:10.1111/j.1600-0625.2011.01433.x
PMID:22379965
Abstract

Itch accompanies various skin diseases. As a number of mediators other than histamine can be involved in the itch sensation, H1 receptor antagonists are not necessarily effective in treating itch. External application of antipruritic drugs is occasionally used as an alternative therapy for pruritic skin conditions, such as pruritus on primary non-diseased, non-inflamed skin. Even so, the actual effects of these drugs on the itch sensation have yet to be studied in detail. To verify the antipruritic effects of crotamiton, capsaicin, and a corticosteroid on the itch sensation, we examined the inhibitory effects of these drugs on various pruritogen-induced scratching behaviors in mice. Topical application of 10% crotamiton moderately inhibited histamine-, serotonin-, and PAR-2 agonist-induced scratching behaviors. Topical capsaicin (0.025%) also exerted a moderate suppressive effect on histamine-, substance P-, and PAR-2 agonist-induced itch responses. Notably, topical corticosteroid (0.05% clobetasol propionate) remarkably inhibited the scratching behaviors induced by all of the pruritogenic agents tested. Therapeutic effects of capsaicin on substance P-induced pruritus did not seem to be mediated by desensitization of the TRPV1 (+) C fibers and/or by altered responsiveness of the mast cells. In addition, the antipruritic effects of crotamiton and corticosteroid appear to be, at least partly, associated with a TRPV1-independent pathway. This study examined the itch responses to pruritogens and demonstrated the mode of action of the externally applied antipruritic drugs.

摘要

瘙痒伴随着各种皮肤病。由于除了组织胺之外还有许多介质可以参与瘙痒感觉,H1 受体拮抗剂在治疗瘙痒方面不一定有效。止痒药物的外用偶尔被用作瘙痒性皮肤病的替代疗法,例如原发性非疾病、非炎症性皮肤的瘙痒。即便如此,这些药物对瘙痒感觉的实际效果尚未详细研究。为了验证克罗他米通、辣椒素和皮质类固醇对瘙痒的止痒作用,我们检查了这些药物对小鼠各种致痒原诱导的搔抓行为的抑制作用。10%克罗他米通的局部应用适度抑制了组胺、血清素和 PAR-2 激动剂诱导的搔抓行为。局部辣椒素(0.025%)也对组胺、P 物质和 PAR-2 激动剂诱导的瘙痒反应产生适度的抑制作用。值得注意的是,局部皮质类固醇(0.05%丙酸氯倍他索)显著抑制了所有测试的致痒原诱导的搔抓行为。辣椒素对 P 物质诱导的瘙痒的治疗效果似乎不是通过 TRPV1(+)C 纤维的脱敏和/或肥大细胞的反应性改变来介导的。此外,克罗他米通和皮质类固醇的止痒作用至少部分与 TRPV1 无关的途径有关。本研究检查了致痒原的瘙痒反应,并证明了外用止痒药物的作用模式。

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