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内皮素B激动剂IRL 1620的体内血流动力学和变力作用

In vivo hemodynamic and inotropic effects of the endothelinB agonist IRL 1620.

作者信息

Beyer M E, Slesak G, Hoffmeister H M

机构信息

Medizinische Klinik, Abteilung III, Eberhard-Karls-Universität, Tübingen, Germany.

出版信息

J Cardiovasc Pharmacol. 1995;26 Suppl 3:S190-2.

PMID:8587359
Abstract

The endothelinB (ETB) receptor is involved in endothelin-induced vasoconstriction and appears to play a role in ET-induced positive inotropy. Our previous study could not detect a positive inotropic effect of ET-1 in vivo. To evaluate specifically the effects of the ETB receptor on hemodynamics and inotropy of ET-1 in the intact circulation, we examined in the open-chest rat model the dose-dependent hemodynamic and inotropic effects of the highly specific ETB agonist IRL 1620 (0.4, 1.0, 2.0, and 4.0 nmol/kg vs. NaCl controls) during and after a 7-min infusion. In addition to measurements in the intact circulation, isovolumic recordings (peak LVSP, peak dP/dtmax) were performed for quantification of myocardial contractility independently of peripheral vascular changes. IRL 1620 caused a significant biphasic blood pressure response with an initial fall and a sustained increase, reflecting the vasoactive effects of IRL 1620, with a transient vasorelaxation followed by dose-dependent and long-lasting vasoconstriction. Although IRL 1620 has a positive chronotropic effect the reduction in stroke volume (probably due to the elevated afterload) causes a decrease in cardiac output. Nevertheless, the isovolumic measurements indicate a significant positive inotropic effect of IRL 1620. Therefore, the selective activation of ETB receptors causes a positive inotropic effect, which is also detectable in vivo, as the vasoconstrictor and coronary constrictor effects are less pronounced compared to activation of both ETA and ETB receptors by ET-1.

摘要

内皮素B(ETB)受体参与内皮素诱导的血管收缩,并且似乎在ET诱导的正性肌力作用中发挥作用。我们之前的研究未能在体内检测到ET-1的正性肌力作用。为了具体评估ETB受体对完整循环中ET-1的血流动力学和正性肌力作用的影响,我们在开胸大鼠模型中,在输注7分钟期间及之后,研究了高特异性ETB激动剂IRL 1620(0.4、1.0、2.0和4.0 nmol/kg,与氯化钠对照组相比)的剂量依赖性血流动力学和正性肌力作用。除了在完整循环中进行测量外,还进行了等容记录(左心室收缩压峰值、最大dp/dt),以独立于外周血管变化来定量心肌收缩力。IRL 1620引起了显著的双相血压反应,最初下降然后持续升高,反映了IRL 1620的血管活性作用,先是短暂的血管舒张,随后是剂量依赖性和持久的血管收缩。尽管IRL 1620具有正性变时作用,但每搏输出量的减少(可能是由于后负荷升高)导致心输出量下降。然而,等容测量表明IRL 1620具有显著的正性肌力作用。因此,ETB受体的选择性激活会引起正性肌力作用,这在体内也可检测到,因为与ET-1同时激活ETA和ETB受体相比,其血管收缩和冠状动脉收缩作用不太明显。

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