Further evidence for the existence of NK2 tachykinin receptor subtypes

Abstract

1 We have evaluated the biological activity of a number of neurokinin A (4–10), (NKA (4–10)) analogues in the endothelium-deprived rabbit isolated pulmonary artery (RPA) and hamster isolated trachea (HT), two tissues rich in different NK₂ receptor subtypes. 2 MDL 28,564, a pseudopeptide selective for NK₂ receptor sites, behaved as a full agonist in the RPA, while in the HT it competitively antagonized NKA or [βAla⁸]-NKA (4–10) contractile effects. 3 The peculiar behaviour of MDL 28,564 in the RPA and HT may be explained neither by a difference in receptor reserve between the two organs (the reserve being three times greater in RPA than in the HT) nor by a different affinity for the two receptor subtypes (identical dissociation constants, pK_A or pK_B, calculated in the RPA and in the HT). On the other hand, MDL 28,564 displayed a very different intrinsic efficacy for the two receptor subtypes. 4 The novel peptides MEN 10,295 ([Trp⁷, βAla⁸]-NKA-(4–10)) and MEN 10,296 ([Tyr⁵, Trp⁷, βAla⁸]-NKA-(4–10)) behaved as weaker agonists than MDL 28,564 in the RPA, but retained appreciable agonist activity also in the HT. 5 The novel peptides: MEN 10,282 ([Tyr⁵, d-Trp^6,8, Trp⁹, Arg¹⁰]-NKA-(4–10)), MEN 10,449 ([diI-Try⁵, d-Trp^6,8,9, Arg¹⁰]-NKA-(4–10)) and the cyclic hexapeptide L 659,877 (cyclo [Leu-Met-Gln-Trp-Phe-Gly]) behaved as competitive antagonists against NKA contractile effects both in the RPA and HT. MEN 10,282 and MEN 10,449 were unable to distinguish between the NK₂ receptor subtypes, having almost the same affinity in the two organs. On the other hand L 659,877 was about 15 times more potent in the HT than in the RPA. 6 These results provide further evidence for NK₂ receptors heterogeneity and are useful in outlining pharmacological features of the two subtypes present in the RPA and HT.