Pharmacological specificity of novel, synthetic, cyclic peptides as antagonists at tachykinin receptors

Abstract

1 The interaction at tachykinin receptors of a series of novel cyclic hexapeptides has been examined by use of radioligand binding assays (NK₁ and NK₃ sites in rat cortex, NK₂ sites in hamster urinary bladder) and functional pharmacological assays (guinea-pig ileum, rat vas deferens and rat portal vein for NK₁, NK₂ and NK₃ receptors, respectively). 2 The compounds cyclc(GlnTrpPhe(R)Gly[ANC-2]LeuMet) (L-659,837) and cyclo(GlnTrpPheGlyLeuMet) (L-659,877) were powerful and selective displacers of NK₂ binding (pIC₅₀ 6.9 and 8.0, respectively), and were competitive antagonists of responses to stimulation of NK₂ receptors in rat vas deferens (pK_B for antagonism of responses to eledoisin 6.7 and 8.1, respectively). Responses in the NK₁ and NK₃ pharmacological assays were blocked only weakly, if at all. 3 In the longitudinal muscle of the small intestine of the rat, responses to stimulation of the putative NK₂ receptor by eledoisin, neurokinin A or neurokinin B were antagonized by both cyclo(GlnTrpPhe(R)Gly[ANC-2]LeuMet) and cyclo(GlnTrpPheGlyLeuMet) in a manner consistent with the presence in this tissue of a uniform population of receptors, indistinguishable from the NK₂ receptor of the rat vas deferens. 4 The compounds cyclo(GlnTrpPheGlyLeuMet) and the lactam-containing analogue are among the most selective antagonists for the NK₂ receptor that have been described; their availability should be of value in the characterization of the receptors mediating responses to tachykinins, and in elucidating the physiological functions of the tachykinin receptors.