Mechanisms of 17 β-oestradiol induced vasodilatation in isolated pressurized rat small arteries

1 The influence of 17 beta-oestradiol on pressurized isolated rat mesenteric and coronary small arteries was investigated. 2 17 beta-oestradiol caused rapid (t(1.0)<5 mins) concentration-dependent relaxations of pre-contracted pressurized (50 mmHg) isolated rat mesenteric and coronary arteries. Similar responses were observed in both vessel types. Significant relaxations were only observed at concentrations exceeding 3 mu M. 3 The vasodilatory responses in both types of artery were unaffected by 10 mu M L-nitro arginine (L-NNA) alone or in the presence of 10 mu M indomethacin, inhibitors of nitric oxide and prostaglandin synthesis respectively. They were also unaffected by the pre-contracting agent used i.e. high K+ or U46619 (a thromboxane analogue). 4 Neither the oestrogen receptor antagonist ICI 182,780 (10 mu M) nor the protein synthesis inhibitor cycloheximide (100 mu M) had any effect on the responses of mesenteric arteries to 17 beta-oestradiol. 5 17 alpha-oestradiol had only a minor effect on mesenteric arterial diameter over a concentration range similar to the effective vasodilatory range for 17 beta-oestradiol. 6 Membrane impermeant 17 beta-oestradiol conjugated to bovine serum albumin (beta-oestradiol-17-hemisuccinate-BSA) (E-H-BSA) resulted in a vasodilatation of pressurized arteries. 7 Wortmannin, an inhibitor of myosin light chain kinase, near maximally relaxed pressurized mesenteric arteries although the time course for the response was significantly slower than that for 17 beta-oestradiol. 8 These results taken together suggest that the acute effects of 17 beta-oestradiol on isolated pressurized arterial tone may be due to effects directly on the vascular smooth muscle via nongenomic mechanisms that involve a stereospecific interaction at the plasma membrane.