Inhibitory effect of noradrenaline uptake inhibitors on contractions of rat aortic smooth muscle

Abstract

1 The effects of noradrenaline (NA) uptake inhibitors on contractions induced by NA, high K⁺, and 12-O-tetradecanoylphorbol-13-acetate (TPA) in rat isolated aorta were investigated. 2 Protriptyline (0.3 μm) and amitriptyline (0.3 μm) produced an approximately parallel shift to the right in the dose-response curve to NA. Protriptyline (>0.3 μm), amitriptyline (>0.3 μm) and xylamine (0.01-1 μm) significantly reduced the maximal contractile response to NA. The IC₅₀ values for inhibition of the contractile response to 3 μm NA were 1.58 μm for xylamine, 1.70 μm for amitriptyline and 2.57 μm for protriptyline. 3 Protriptyline and amitriptyline dose-dependently inhibited the high K⁺ (60 mM)-induced contraction (IC₅₀ = 0.69 μm for protriptyline and IC₅₀ = 3.15 μm for amitriptyline). In contrast, xylamine did not affect the high K(⁺-induced contraction. 4 Protriptyline and amitriptyline dose-dependently inhibited TPA (1 μm)-induced contraction in calcium-free solution; xylamine (up to 30 μm) was without effect. Staurosporine (10 nM) completely inhibited the TPA- and NA-induced contraction. 5 Protriptyline (3 μm) and amitriptyline (3 μm) caused about 54% and 60% inhibition, respectively, of aortic contractions caused by endothelin-1 (10 nM) in the absence of endothelium. Xylamine (10 μm) was without effect. 6 Inhibitory effects of NA uptake inhibitors on contractions were independent of the presence of endothelium and were unaffected by the K⁺ channel blockers, tetraethylammonium ions (up to 3 mM) and glibenclamide (up to 30 μm). 7 These results indicate that tricyclic antidepressant drugs such as protriptyline and amitriptyline could act as both postsynaptic adrenoceptor antagonists and direct inhibitors of muscle contraction; whereas, xylamine, a structurally distinct NA uptake blocker might principally exert its action only at α-adrenoceptors on rat aortic smooth muscle.