维拉帕米在心肌缺血和再灌注期间的心肌保护作用：心肌挽救与缺血期间ATP耗竭程度之间的分离。

Myocardial protection with verapamil during ischaemia and reperfusion: dissociation between myocardial salvage and the degree of ATP depletion during ischaemia.

作者信息

Wolfe C L, Donnelly T J, Sievers R, Parmley W W

机构信息

Department of Internal Medicine (Cardiology), University of California San Francisco, Moffitt Hospital 94143-0124.

出版信息

Cardiovasc Res. 1991 Feb;25(2):101-9. doi: 10.1093/cvr/25.2.101.

DOI:10.1093/cvr/25.2.101

PMID:1742760

Abstract

STUDY OBJECTIVE

The aim was to evaluate the protective effect of verapamil during myocardial ischaemia and reperfusion.

DESIGN

In vivo phosphorus-31 (31P) magnetic resonance spectroscopy was performed on rats pretreated with verapamil (mg.kg-1 intraperitoneal) and controls during a 45 min left coronary artery occlusion and 60 min reperfusion. In separate groups of animals, haemodynamic measurements were taken at baseline, during ischaemia, and during reperfusion. Infarct size was determined by staining with triphenyltetrazolium chloride.

EXPERIMENTAL MATERIAL

Female Sprague-Dawley rats were used (control group n = 25, experimental group n = 24).

MEASUREMENTS AND MAIN RESULTS

Infarct size was significantly reduced in the verapamil group compared to controls: 9.9(SEM 2.3)%, n = 19 v 28.5(2.7)%, n = 19, p less than 0.001 (infarct % of left ventricular mass). Myocardial phosphocreatine and ATP levels were reduced to similar levels in both verapamil and control animals after 45 min ischaemia: 56.8(3.4)%, n = 10, v 61.4(1.8)%, n = 11 NS; 67.7(2.7)%, n = 10 v 69.7(2.9)%, n = 11, NS (% of baseline value). After 60 min reflow, there was significant recovery of phosphocreatine [91.1(4.2)% of baseline, p less than 0.05] and ATP [86.8(2.7)% of baseline, p less than 0.05] in the verapamil group, but no recovery of high energy phosphates in controls [66.3(2.8), NS; 69.6(2.7), NS]. The left ventricular systolic pressure, heart rate, rate-pressure product, and maximum rate of left ventricular pressure development were similar prior to ischaemia, and during ischaemia in both groups. There was an inverse correlation between infarct size and the degree of phosphocreatine recovery after 60 min of reperfusion (PCr recovery (%) = -0.99 x infarct size (%) + 101; r = 0.91; p less than 0.01; n = 14). Furthermore, in a separate group of animals (n = 9), there was a significant correlation between the size of the ischaemic area at risk and the degree of phosphocreatine decline after 15 min of coronary occlusion (PCr reduction (%) = 0.91 x risk area (%) + 5.6; r = 0.97; p less than 0.01).

CONCLUSIONS

Pretreatment with verapamil extends the ischaemic time after which reperfusion results in myocardial salvage in this model of ischaemia and reperfusion. This protective effect is independent of the haemodynamic determinants of myocardial oxygen demand and the degree of ATP and phosphocreatine depletion during the ischaemic period. In this model of reversible ischaemia, 31P magnetic resonance spectroscopy is useful for quantitating both the size of the ischaemic region during coronary artery occlusion and infarct size after reperfusion.

摘要

研究目的

旨在评估维拉帕米在心肌缺血及再灌注过程中的保护作用。

设计

对经维拉帕米（腹腔注射，mg.kg-1）预处理的大鼠及对照组大鼠在左冠状动脉闭塞45分钟及再灌注60分钟期间进行体内磷-31（31P）磁共振波谱分析。在不同组动物中，于基线、缺血期间及再灌注期间进行血流动力学测量。梗死面积通过氯化三苯基四氮唑染色确定。

实验材料

使用雌性斯普拉格-道利大鼠（对照组n = 25，实验组n = 24）。

测量指标及主要结果

与对照组相比，维拉帕米组梗死面积显著减小：9.9（标准误2.3）%，n = 19 对比 28.5（2.7）%，n = 19，p < 0.001（梗死面积占左心室质量的百分比）。缺血45分钟后，维拉帕米组和对照组心肌磷酸肌酸及ATP水平均降至相似水平：56.8（3.4）%，n = 10 对比 61.4（1.8）%，n = 11，无显著差异；67.7（2.7）%，n = 10 对比 69.7（2.9）%，n = 11，无显著差异（占基线值的百分比）。再灌注60分钟后，维拉帕米组磷酸肌酸[占基线的91.1（4.2）%，p < 0.05]和ATP[占基线的86.8（2.7）%，p < 0.05]有显著恢复，但对照组高能磷酸盐无恢复[66.3（2.8），无显著差异；69.6（2.7），无显著差异]。两组在缺血前及缺血期间左心室收缩压、心率、心率-压力乘积及左心室压力上升最大速率相似。再灌注60分钟后梗死面积与磷酸肌酸恢复程度呈负相关（磷酸肌酸恢复（%）= -0.99×梗死面积（%）+ 101；r = 0.91；p < 0.01；n = 14）。此外，在另一组动物（n = 9）中，冠状动脉闭塞15分钟后缺血危险区域大小与磷酸肌酸下降程度之间存在显著相关性（磷酸肌酸降低（%）= 0.91×危险区域（%）+ 5.6；r = 0.97；p < 0.01）。