Structure activity studies of mast cell activation and hypotension induced by neuropeptide Y (NPY), centrally truncated and C‐terminal NPY analogues

Abstract

1 Neuropeptide-induced histamine release is thought to occur via receptor-independent mechanisms, with net charge and lipophilicity being important factors. 2 In this study, the histamine releasing ability of neuropeptide Y (NPY), two C-terminal segments of NPY and 13 centrally truncated NPY analogues was examined. These results were compared with the ability of the peptides to bind to the Y₂ receptor in the rabbit kidney membrane model and with their hypotensive actions in the anaesthetized-rat model. 3 All analogues tested, with the exception of [Glu^4,25,33,35]-NPY(1–4)-Ahx-(25–36) and [Asp^4,25,33,35]NPY(1–4)-Ahx-(25–36) which were devoid of histamine releasing activity, evoked a dose-dependent histamine release but there were marked differences between the peptides. The native peptide was the least active. 4 Histamine release was not linked to the ability of the peptides to displace NPY from Y₂ receptors. There was a statistical correlation between the hypotensive effects expressed as ED₁₀ values (μmol kg⁻¹, which induced a blood pressure decrease of 10 mmHg) and the EC₂₅ for histamine release (r = 0.62, P = 0.04), although histamine release may not be the sole determinant of the alterations in blood pressure. 5 There was a strong negative correlation between EC₂₅ for histamine release and net positive charge (r = −0.93, P = 5.7 × 10⁻⁷), i.e. increasing the net positive charge caused greater histamine release. However, there was a 12 fold difference in activity amongst the most positively charged analogues (+ 5). Helicity did not correlate with histamine releasing ability. 6 In the development of NPY-related drugs the avoidance of compounds with net positive charge is recommended.