Evidence that mechanisms dependent and independent of nitric oxide mediate endothelium-dependent relaxation to bradykinin in human small resistance-like coronary arteries

1 The effects of the nitric oxide (NO) synthase inhibitor, N-G-nitro-L-arginine (L-NOARG), the NO scavenger, oxyhaemoglobin (HbO) and high extracellular K+ upon endothelium-dependent relaxation to bradykinin were investigated in human isolated small coronary arteries. 2 Endothelium-dependent relaxations to bradykinin were compared in vessels contracted to similar to 50% of their maximum contraction to 124 mM KCI Krebs solution, regardless of treatments, with the thromboxane A(2) mimetic, U46619 and acetylcholine. All relaxations were expressed as percentage reversal of the initial level of active force. 3 L-NOARG (100 mu M) caused a small but significant, 12% (P<0.01), decrease in the maximum relaxation (R(max): 91.5+/-5.4%) to bradykinin but did not significantly affect the sensitivity (pEC(50): 8.08+/-0.17). Increasing the concentration of L-NOARG to 300 mu M had no further effect on the pEC(50) or R(max) to bradykinin. HbO (20 mu M) and a combination of HbO (20 mu M) and L-NOARG (100 mu M) reduced R(max) to bradykinin by 58% (P<0.05) and 54% (P<0.05), respectively. HbO (20 mu M) and L-NOARG (100 mu M, combined but not HbO (20 mu M) alone, caused a significant 11 fold (P<0.05) decrease in sensitivitiy to bradykinin. HbO (20 mu M) decreased the sensitivity to the endothelium-independent NO donor, S-nitroso-N-acetylpenicillamine (SNAP), approximately 17 fold (P<0.05). 4 Raising the extracellular concentration of K+ isotonically to 30 mM, reduced the R(max) to bradykinin from 96.6+/-3.1% to 43.9+/-10.1% (P<0.01) with no significant change in sensitivity. A combination of HbO, L-NOARG and high K+ (30 mM) abolished the response to bradykinin. High K+ did not change either the sensitivity or maximum relaxation to SNAP. 5 In conclusion, L-NOARG does not completely inhibit endothelial cell NO synthesis in human isolated small coronary arteries. By comparison, HbO appeared to block all the effects of NO in this tissue and revealed that most of the relaxation to bradykinin was due to NO. The non-NO -dependent relaxation to bradykinin in the human isolated small coronary arteries appeared to be mediated by a K+-sensitive vasodilator mechanism, possibly endothelium-derived hyperpolarizing factor (EDHF).