麻醉猪体内钾通道激活剂EMD 52692的血流动力学特征

Haemodynamic profile of the potassium channel activator EMD 52692 in anaesthetized pigs.

作者信息

Sassen L M, Duncker D J, Gho B C, Diekmann H W, Verdouw P D

机构信息

Laboratory for Experimental Cardiology (Thoraxcentre), Erasmus University Rotterdam, The Netherlands.

出版信息

Br J Pharmacol. 1990 Nov;101(3):605-14. doi: 10.1111/j.1476-5381.1990.tb14128.x.

DOI:10.1111/j.1476-5381.1990.tb14128.x

PMID:2076480

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1917749/

Abstract

The systemic and regional haemodynamic effects of the potassium channel activator EMD 52692 or its solvent were investigated after intravenous and after intracoronary administration in anaesthetized pigs. 2. Consecutive intravenous 10 min infusions of EMD 52692 (0.15, 0.30, 0.60, 1.20 micrograms kg-1 min-1; n = 7) dose-dependently decreased mean arterial blood pressure by up to 50%. This was entirely due to peripheral vasodilatation, since cardiac output did not change. Heart rate increased by up to 50%, while left ventricular end diastolic pressure decreased dose-dependently from 6 +/- 1 mmHg to 3 +/- 1 mmHg (P less than 0.05), and stroke volume decreased from 30 +/- 2 ml to 21 +/- 2 ml (P less than 0.05). Left ventricular dP/dtmax was not affected. 3. Although cardiac output did not change, EMD 52692 caused a redistribution of blood flow from the arteriovenous anastomoses to the capillary channels. Blood flow to the adrenals, small intestine, stomach, bladder, spleen and brain increased, while renal blood flow decreased and blood flow to several muscle groups and skin were not altered. Vascular conductance was increased dose-dependently in all organs, except for the kidneys, where after the initial increase, vascular conductance returned to baseline with the highest dose. Particularly striking were the effects on the vasculature of the brain. With the highest dose of EMD 52692 blood flow more than doubled, while vascular conductance increased four fold. 4. Transmural myocardial blood flow increased slightly, which was entirely due to an increase in subepicardial blood flow. Myocardial O2-consumption and segment length shortening were not significantly affected. 5. After consecutive 10 min intracoronary infusions (0.0095, 0.019, 0.0375 and 0.075 microgram kg-1 min-1; n = 7) into the left anterior descending coronary artery (LADCA), mean arterial blood pressure was maintained with the lowest two doses, but decreased by up to 15% with the higher doses, whereas heart rate increased by up to 24%. Blood flow to the LADCA-perfused myocardium doubled with the highest dose, the subepicardium benefitting the most. Coronary venous O2-saturation increased dose-dependently from 23 +/- 2% to 60 +/- 4%, while myocardial O2-consumption of the LADCA-perfused myocardium was not affected by the drug. 6. It is concluded that EMD 52692 is a potent vasodilator, with particularly pronounced effects on vasculature of the brain. Its selectivity for vascular smooth muscle cells exceeds that for the myocytes, since with doses that are much higher than those of potential clinical interest no negative inotropic effects were observed. The compound primarily dilates arteries but some venodilatation may also occur.

摘要

在麻醉猪身上静脉内和冠状动脉内给药后，研究了钾通道激活剂EMD 52692或其溶剂的全身和局部血流动力学效应。2. 连续静脉输注EMD 52692（0.15、0.30、0.60、1.20微克·千克⁻¹·分钟⁻¹；n = 7）10分钟，剂量依赖性地使平均动脉血压降低高达50%。这完全是由于外周血管扩张，因为心输出量没有变化。心率增加高达50%，而左心室舒张末期压力从6±1毫米汞柱剂量依赖性地降至3±1毫米汞柱（P<0.05），每搏输出量从30±2毫升降至21±2毫升（P<0.05）。左心室dP/dtmax未受影响。3. 虽然心输出量没有变化，但EMD 52692导致血流从动静脉吻合处重新分布到毛细血管通道。肾上腺、小肠、胃、膀胱、脾脏和大脑的血流量增加，而肾血流量减少，几个肌肉群和皮肤的血流量未改变。除肾脏外，所有器官的血管传导率均呈剂量依赖性增加，在肾脏中，最初增加后，血管传导率在最高剂量时恢复到基线水平。对脑血管系统的影响尤为显著。使用最高剂量的EMD 52692时，血流量增加了一倍多，而血管传导率增加了四倍。4. 透壁心肌血流量略有增加，这完全是由于心外膜下血流量增加。心肌耗氧量和节段长度缩短未受显著影响。5. 连续10分钟向冠状动脉左前降支（LADCA）内输注（0.0095、0.019、0.0375和0.075微克·千克⁻¹·分钟⁻¹；n = 7）后，最低的两个剂量可维持平均动脉血压，但较高剂量可使其降低高达15%，而心率增加高达24%。最高剂量时，LADCA灌注心肌的血流量增加了一倍，心外膜下受益最大。冠状静脉血氧饱和度从23±2%剂量依赖性地增加到60±4%，而LADCA灌注心肌的心肌耗氧量不受该药物影响。6. 结论是，EMD 52692是一种强效血管扩张剂，对脑血管系统有特别显著的影响。它对血管平滑肌细胞的选择性超过对心肌细胞的选择性，因为在远高于潜在临床应用剂量的情况下未观察到负性肌力作用。该化合物主要扩张动脉，但也可能发生一些静脉扩张。