A bradykinin (BK)1 receptor antagonist blocks capsaicin‐induced ear inflammation in mice
Open Access
- 1 March 1990
- journal article
- research article
- Published by Wiley in British Journal of Pharmacology
- Vol. 99 (3) , 516-518
- https://doi.org/10.1111/j.1476-5381.1990.tb12960.x
Abstract
1 The effect of various peptide antagonists on capsaicin-induced (250 μg per ear) ear inflammation has been examined. 2 Co-administration of the substance P (SP) antagonist [d-Pro2,d-Trp7,9]SP at 100 and 300 μg per ear with capsaicin markedly attenuated oedema, whereas a vasopressin antagonist was ineffective. 3 Using the same scheme, the mixed BK2 and BK1 bradykinin (BK) antagonist NPC 567 (d-Arg[Hyp3, d-Phe7]BK) did not inhibit oedema at 100 μg per ear, but did inhibit at a higher dose (300 μg). The BK1 antagonist [Leu8,desArg9]BK produced significant inhibition at both doses. 4 When BK was used to induce ear inflammation (30 μg per ear), the SP antagonist inhibited ear oedema. Both BK receptor subtype antagonists inhibited inflammation with the BK1 being more potent than the BK2 antagonist. 5 These results suggest that BK1 along with BK2 receptors are located on capsaicin-sensitive fibres, where they may modulate the degree of neurogenic inflammation.This publication has 11 references indexed in Scilit:
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