Non-peptide antagonists, CP-96,345 and RP 67580, distinguish species variants in tachykinin NK1 receptors

Abstract

1 The potency of the non-peptide antagonists CP-96,345 and RP 67580 on NK₁ receptor-stimulated [³H]-inositol phosphate accumulation in cell lines or tissue from three different species has been examined. 2 We have used: UC11 cells, derived from a human astrocytoma, and rat LRM55 glial cells, both of which express large numbers of functional NK₁ receptors, and the well characterized guinea-pig ileum which expresses both NK₁ and NK₃ receptors. 3 RP 67580 has an ∼25 fold lower affinity for NK₁ receptors in human UC11 cells (Kd = 194 nm) than in rat LRM55 cells (Kd = 7.9 nm), in contrast CP-96,345 has an ∼200 fold lower affinity in rat LRM55 cells (Kd = 210 nm) relative to human UC11 cells (Kd = 0.99 nm). The pharmacological profile of CP-96,345 and RP 67580 in guinea-pig ileum was similar to that observed in human UC11 cells. 4 In conclusion, we have demonstrated that previously reported species differences in binding affinities for the non-peptide NK₁ antagonists, CP-96,345 and RP 67580, are also observed in inhibition of NK₁ receptor stimulated hydrolysis of inositol phospholipids.