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舒马曲坦的中枢或外周作用对炎性和非炎性内脏痛的逆转作用。

Reversal of inflammatory and noninflammatory visceral pain by central or peripheral actions of sumatriptan.

作者信息

Vera-Portocarrero Louis P, Ossipov Michael H, King Tamara, Porreca Frank

机构信息

Department of Pharmacology, College of Medicine, University of Arizona, Health SciencesCenter, Tucson, Arizona 85724, USA.

出版信息

Gastroenterology. 2008 Oct;135(4):1369-78. doi: 10.1053/j.gastro.2008.06.085. Epub 2008 Jul 3.

Abstract

BACKGROUND & AIMS: Sumatriptan is used specifically to relieve headache pain. The possible efficacy of sumatriptan was investigated in 2 models of visceral pain.

METHODS

Pancreatic inflammation was induced by intravenous injection of dibutyltin dichloride. Noninflammatory irritable bowel syndrome was induced by intracolonic instillation of sodium butyrate. The effects of systemic sumatriptan on referred hypersensitivity were tested in both models. Effects of sumatriptan within the rostral ventromedial medulla (RVM), a site of descending modulation of visceral pain, was determined by (1) testing the effects of RVM administration of 5HT1(B/D) antagonists on systemic sumatriptan action and (2) determining whether RVM application of sumatriptan reproduced the actions of systemic drug administration.

RESULTS

Systemic sumatriptan elicited a dose- and time-related blockade of referred hypersensitivity in both models that was blocked by systemic administration of either 5HT1(B) or 5HT1(D) antagonists. Sumatriptan administered into the RVM similarly produced dose- and time-related blockade of referred hypersensitivity in both visceral pain models. This was blocked by local microinjection of the 5HT1(B) antagonist but not the 5HT1(D) antagonist. Microinjection of 5HT1(B) or 5HT1(D) antagonists into the RVM did not block the effects of systemic sumatriptan.

CONCLUSIONS

Our findings suggest that sumatriptan suppresses either inflammatory or noninflammatory visceral pain, most likely through peripheral 5HT1(B)/(D) receptors. Actions at 5HT1(B) receptors within the RVM offer an additional potential site of action for the modulation of visceral pain by triptans. These studies offer new insights into the development of strategies that may improve therapy of visceral pain conditions using already available medications.

摘要

背景与目的

舒马曲坦专门用于缓解头痛疼痛。在两种内脏痛模型中研究了舒马曲坦的可能疗效。

方法

通过静脉注射二氯化二丁基锡诱导胰腺炎症。通过结肠内注入丁酸钠诱导非炎症性肠易激综合征。在两种模型中测试了全身应用舒马曲坦对牵涉性超敏反应的影响。通过以下方式确定舒马曲坦在内侧延髓头端腹内侧(RVM)(内脏痛下行调制部位)的作用:(1)测试RVM给予5HT1(B/D)拮抗剂对全身应用舒马曲坦作用的影响,以及(2)确定RVM应用舒马曲坦是否重现全身给药的作用。

结果

在两种模型中,全身应用舒马曲坦均引起剂量和时间相关的牵涉性超敏反应阻断,这被全身给予5HT1(B)或5HT1(D)拮抗剂所阻断。在两种内脏痛模型中,向RVM注射舒马曲坦同样产生剂量和时间相关的牵涉性超敏反应阻断。这被5HT1(B)拮抗剂的局部微量注射所阻断,但未被5HT1(D)拮抗剂阻断。向RVM微量注射5HT1(B)或5HT1(D)拮抗剂并未阻断全身应用舒马曲坦的作用。

结论

我们的研究结果表明,舒马曲坦最有可能通过外周5HT1(B)/(D)受体抑制炎症性或非炎症性内脏痛。RVM内5HT1(B)受体的作用为曲坦类药物调节内脏痛提供了另一个潜在作用位点。这些研究为开发可能利用现有药物改善内脏痛治疗策略提供了新的见解。

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