实验性充血性心力衰竭中内皮素-B受体激活导致的冠状动脉血管收缩增强。

Enhanced coronary vasoconstriction to endothelin-B-receptor activation in experimental congestive heart failure.

作者信息

Cannan C R, Burnett J C, Lerman A

机构信息

Department of Internal Medicine and Physiology, Mayo Clinic/Foundation, Rochester, Minn 55905, USA.

出版信息

Circulation. 1996 Feb 15;93(4):646-51. doi: 10.1161/01.cir.93.4.646.

DOI:10.1161/01.cir.93.4.646

PMID:8640990

Abstract

BACKGROUND

Endothelin (ET), a coronary vasoconstrictor, mediates its activity through the specific receptors ET-A and ET-B, which may demonstrate different activity under pathophysiological conditions. Thoracic inferior vena cava constriction (TIVCC) is an experimental model of congestive heart failure that is characterized by a decrease in cardiac output and an increase in circulating ET concentrations. The present study was designed to test the hypothesis that experimental heart failure altered coronary vascular responsiveness to ET-A- and ET-B-receptor stimulation in vivo.

METHODS AND RESULTS

ET-1 was infused at a rate of 2 ng/kg per minute into the left circumflex coronary artery in normal dogs (n = 5) and in dogs subjected to TIVCC (TIVCC dogs, n = 6). Similarly, sarafotoxin, an ET-B-receptor agonist, was infused at the same dosage in normal (n = 5) and TIVCC (n = 6) dogs. Intracoronary infusion of ET-1 significantly decreased coronary blood flow and increased coronary vascular resistance in normal dogs; this effect was significantly attenuated in TIVCC compared with normal dogs. The percent changes in coronary blood flow and coronary vascular resistance in the TIVCC compared with the normal dogs was -11 +/- 8% versus -48 +/- 7% (P < .01) and 29 +/- 10% versus 105 +/- 23% (P < .01), respectively. There was no significant effect on coronary blood flow, coronary vascular resistance, or coronary artery diameter in normal dogs that received an intracoronary infusion of sarafotoxin. In contrast, the administration of intracoronary sarafotoxin in TIVCC compared with normal dogs resulted in significant percent changes in coronary blood flow and coronary vascular resistance (-31 +/- 4% versus -7 +/- 3% [P < .001] and 53 +/- 12% versus 12 +/- 8% [P < .02], respectively).

CONCLUSIONS

The present study demonstrates an attenuated coronary vasoconstrictor response to ET-1 with an enhanced vasoconstrictor response to sarafotoxin and suggests an alteration in coronary ET receptor sensitivity in experimental heart failure.

摘要

背景

内皮素（ET）是一种冠状动脉收缩剂，通过特异性受体ET - A和ET - B介导其活性，在病理生理条件下这两种受体可能表现出不同的活性。胸段下腔静脉缩窄（TIVCC）是一种充血性心力衰竭的实验模型，其特征是心输出量减少和循环ET浓度增加。本研究旨在验证实验性心力衰竭会改变体内冠状动脉对ET - A和ET - B受体刺激的血管反应性这一假设。

方法与结果

以每分钟2 ng/kg的速率将ET - 1注入正常犬（n = 5）和接受TIVCC的犬（TIVCC犬，n = 6）的左旋冠状动脉。同样，以相同剂量将ET - B受体激动剂沙拉毒素注入正常犬（n = 5）和TIVCC犬（n = 6）。在正常犬中，冠状动脉内注入ET - 1显著降低冠状动脉血流量并增加冠状动脉血管阻力；与正常犬相比，TIVCC犬的这种作用显著减弱。与正常犬相比，TIVCC犬冠状动脉血流量和冠状动脉血管阻力的百分比变化分别为-11±8%对-48±7%（P <.01）和29±10%对105±23%（P <.01）。冠状动脉内注入沙拉毒素对正常犬的冠状动脉血流量、冠状动脉血管阻力或冠状动脉直径没有显著影响。相比之下，与正常犬相比，TIVCC犬冠状动脉内给予沙拉毒素导致冠状动脉血流量和冠状动脉血管阻力有显著的百分比变化（分别为-31±4%对-7±3% [P <.001]和53±12%对12±8% [P <.02]）。