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维拉帕米对离体大鼠心脏再灌注损伤和钙反常的影响。

Effect of verapamil on reperfusion damage and calcium paradox in isolated rat heart.

作者信息

Alanen K A, Lipasti J A, Tasanne M R, Nevalainen T J

出版信息

Exp Pathol. 1984;25(3):131-8. doi: 10.1016/s0232-1513(84)80031-6.

Abstract

The effect of verapamil on ischaemic contracture, reperfusion injury after global ischaemia, and calcium paradox was studied in isolated rat heart. The development of ischaemic contracture was measured by a balloon catheter inserted into the left ventricle, filled with water, and connected to a pressure recorder. Myocardial perfusability was tested by infusing sodium fluorescein solution into the cannulated aortic root. Creatine kinase (CK) activity and protein leakage from myocardium into the effluent were measured during reperfusion (30 min) after ischaemia (50 min) and during calcium repletion (30 min) after calcium depletion (5 min). Ischaemic contracture developed later in the verapamil-treated group (31.7 +/- 0.7 min) than in the control group (23.6 +/- 2.2 min). There was less CK (29.16 +/- 3.26 U/g) and protein leakage (4.81 +/- 0.41 mg/g) in the verapamil-treated group than in the control group (38.81 +/- 3.30 U/g and 6.14 +/- 0.49 mg/g, respectively) during reperfusion. Verapamil had no effect on the myocardial perfusability or on the strength of the ischaemic contracture. Verapamil did not reduce the CK or protein leakage in calcium paradox. It was concluded that verapamil has some protective effect against cell injury on myocardium during post-ischaemic reperfusion but none in calcium paradox.

摘要

在离体大鼠心脏中研究了维拉帕米对缺血性挛缩、全心缺血后再灌注损伤及钙反常的影响。通过将插入左心室并充满水的球囊导管连接到压力记录仪来测量缺血性挛缩的发展。通过向插管的主动脉根部注入荧光素钠溶液来测试心肌灌注能力。在缺血(50分钟)后的再灌注(30分钟)期间以及钙耗竭(5分钟)后的钙补充(30分钟)期间,测量肌酸激酶(CK)活性以及心肌向流出液中的蛋白渗漏。维拉帕米治疗组缺血性挛缩的出现时间(31.7±0.7分钟)晚于对照组(23.6±2.2分钟)。在再灌注期间,维拉帕米治疗组的CK(29.16±3.26 U/g)和蛋白渗漏(4.81±0.41 mg/g)低于对照组(分别为38.81±3.30 U/g和6.14±0.49 mg/g)。维拉帕米对心肌灌注能力或缺血性挛缩的强度没有影响。维拉帕米在钙反常中未降低CK或蛋白渗漏。得出的结论是,维拉帕米在缺血后再灌注期间对心肌细胞损伤有一定的保护作用,但在钙反常中没有保护作用。

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