A bradykinin (BK)1 receptor antagonist blocks capsaicin‐induced ear inflammation in mice

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-Trp^7,9]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.