Cannan C R, Burnett J C, Brandt R R, Lerman A
Department of Internal Medicine and Physiology, Mayo Clinic/Foundation, Rochester, Minn 55905, USA.
Circulation. 1995 Dec 1;92(11):3312-7. doi: 10.1161/01.cir.92.11.3312.
Endothelin-1 (ET-1) is an endothelium-derived vasoconstrictor peptide. Controversy persists regarding the predominant ET receptor that mediates coronary vasoconstriction at pathophysiological concentrations. The aim of the present study was to test the hypothesis that ET mediates local coronary vasoconstriction via the ET-A receptor at low concentrations of exogenous ET-1 designed to mimic pathophysiological states compared with pharmacological concentrations.
ET-1 (group 1, n = 5) or sarafotoxin, a specific ET-B receptor agonist (group 3, n = 6) (each at 2 ng/kg per minute), was infused into the left circumflex coronary artery in the anesthetized dog. In group 2 dogs (n = 5), the same dose of ET-1 was infused with 4 micrograms/kg per minute of the specific ET-A receptor antagonist FR-139317. In group 4 (n = 5), the same dose of sarafotoxin was infused with 50 micrograms/kg per minute of the specific inhibitor of nitric oxide formation, NG-monomethyl-L-arginine (L-NMMA). No difference in hemodynamics, coronary blood flow (CBF), coronary vascular resistance (CVR), or coronary artery diameter (CAD) was observed at baseline between the groups. In group 1, intracoronary ET-1 significantly decreased CBF and CAD in association with an increase in CVR. The percentage decrease in CBF and CAD in the group that received ET-1 and the ET-A receptor antagonist (group 2) was significantly less than that in the group that received ET-1 alone (group 1) (-12 +/- 3% versus -48 +/- 6% [P < .001] and -4.6 +/- 0.8 versus 1.0 +/- 0.3 [P < .05], respectively). The administration of the ET-A receptor antagonist (group 2) abolished the ET-mediated increase in CVR (7 +/- 5% versus 105 +/- 21%, P < .005). There was no significant effect on CBF, CVR, or CAD in the group receiving sarafotoxin alone (group 3). The administration of L-NMMA and sarafotoxin (group 3). The administration of L-NMMA and sarafotoxin (group 4) resulted in a significant percentage decrease in CBF compared with the group that received sarafotoxin alone (-28 +/- 7% versus -8 +/- 2% [P < .05]).
The present study demonstrates that low concentrations of exogenous ET-1, which may mimic pathophysiological concentrations, result in coronary vasoconstriction mediated predominantly via the ET-A receptor because such vasoconstriction is significantly attenuated by blockade with FR-139317. The ET-B receptor may have a dual vasoconstrictive and vasodilatory effect.
内皮素 -1(ET-1)是一种内皮源性血管收缩肽。关于在病理生理浓度下介导冠状动脉收缩的主要ET受体仍存在争议。本研究的目的是检验以下假设:与药理浓度相比,在旨在模拟病理生理状态的低浓度外源性ET-1情况下,ET通过ET-A受体介导局部冠状动脉收缩。
将ET-1(第1组,n = 5)或特异性ET-B受体激动剂沙罗毒素(第3组,n = 6)(均为每分钟2 ng/kg)注入麻醉犬的左旋冠状动脉。在第2组犬(n = 5)中,以每分钟4 μg/kg的剂量注入相同剂量的ET-1与特异性ET-A受体拮抗剂FR-139317。在第4组(n = 5)中,以每分钟50 μg/kg的剂量注入相同剂量的沙罗毒素与一氧化氮生成的特异性抑制剂NG-单甲基-L-精氨酸(L-NMMA)。各组间基线时的血流动力学、冠状动脉血流量(CBF)、冠状动脉血管阻力(CVR)或冠状动脉直径(CAD)无差异。在第1组中,冠状动脉内注入ET-1显著降低了CBF和CAD,同时CVR增加。接受ET-1和ET-A受体拮抗剂的组(第2组)中CBF和CAD的降低百分比显著低于单独接受ET-1的组(第1组)(分别为-12±3%对-48±6%[P <.001]和-4.6±0.8对1.0±0.3[P <.05])。ET-A受体拮抗剂的给药(第2组)消除了ET介导的CVR增加(7±5%对105±21%,P <.005)。单独接受沙罗毒素的组(第3组)中对CBF、CVR或CAD无显著影响。L-NMMA和沙罗毒素的给药(第4组)导致CBF较单独接受沙罗毒素的组显著降低(-28±7%对-8±2%[P <.05])。
本研究表明,可能模拟病理生理浓度的低浓度外源性ET-1导致主要通过ET-A受体介导的冠状动脉收缩,因为这种血管收缩被FR-139317阻断后显著减弱。ET-B受体可能具有双重血管收缩和血管舒张作用。
