缺血预处理后给予L-精氨酸可增强离体大鼠心脏的心脏保护作用。
L-Arginine given after ischaemic preconditioning can enhance cardioprotection in isolated rat hearts.
作者信息
Suematsu Y, Ohtsuka T, Hirata Y, Maeda K, Imanaka K, Takamoto S
机构信息
Department of Cardiothoracic Surgery, University of Tokyo, 7-3-1 Hongo, Bunkyo-ku, 113-8655, Tokyo, Japan.
出版信息
Eur J Cardiothorac Surg. 2001 Jun;19(6):873-9. doi: 10.1016/s1010-7940(01)00699-6.
OBJECTIVE
Ischaemic or pharmacological preconditioning with L-arginine has been reported to be insufficient for optimal cardioprotection. The ability of nitric oxide (NO) to enhance ischaemic preconditioning was assessed, and the role of L-arginine-induced ischaemic preconditioning in myocardial protection was determined.
METHODS
Isolated rat hearts were prepared and divided into six groups: control hearts (control, n=6) were perfused without global ischaemia at 37 degrees C for 160 min; global ischaemia hearts (GI, n=6) were subjected to ischaemia for 20 min and reperfusion for 120 min; ischaemic preconditioned hearts (IP, n=6) received 2 min of zero-flow global ischaemia followed by 5 min reperfusion, before 20 min of global ischaemia; L-arginine hearts (ARG, n=6) received 1 mmol/l L-arginine for 5 min, before 20 min of global ischaemia; ischaemic preconditioning plus nitro-L-arginine methyl ester hearts (IP+L-NAME, n=6) received 2 min of ischaemic preconditioning and 5 min reperfusion with 3 mmol/l L-NAME in Krebs-Henseleit buffer, before 20 min of global ischaemia; and ischaemic preconditioning plus L-arginine hearts (IP+ARG, n=6) received 2 min of ischaemic preconditioning and 5 min reperfusion with 1 mmol/l L-arginine in Krebs-Henseleit buffer. Haemodynamic parameters and coronary flow were recorded continuously. Nitrites and nitrates (NOx) were measured 5 and 60 min after reperfusion, and infarct size was also determined.
RESULTS
In the IP+ARG group, significant amelioration and preservation of left ventricular peak developed pressure and coronary flow was observed compared with the GI, IP, ARG and IP+L-NAME groups. Infarct size in the IP+ARG group was reduced significantly compared with that in the GI, IP, ARG and IP+L-NAME groups. Significant preservation of NOx was observed during reperfusion in the IP+ARG group compared with the GI group.
CONCLUSIONS
Inhibition of NO synthase with L-NAME had little impact on ischaemic preconditioning, suggesting that endogenous NO is not a major mediator of ischaemic preconditioning. Nevertheless, enhancement of the effects of ischaemic preconditioning can be achieved with L-arginine, a precursor of NO, improving post-ischaemic functional recovery and infarct size in the isolated rat heart.
目的
据报道,用L-精氨酸进行缺血预处理或药物预处理不足以实现最佳的心脏保护。评估一氧化氮(NO)增强缺血预处理的能力,并确定L-精氨酸诱导的缺血预处理在心肌保护中的作用。
方法
制备离体大鼠心脏并分为六组:对照心脏(对照组,n = 6)在37℃下无全心缺血灌注160分钟;全心缺血心脏(GI组,n = 6)缺血20分钟,再灌注120分钟;缺血预处理心脏(IP组,n = 6)在全心缺血20分钟前先进行2分钟零流量全心缺血,然后再灌注5分钟;L-精氨酸心脏(ARG组,n = 6)在全心缺血20分钟前接受1 mmol/L L-精氨酸处理5分钟;缺血预处理加硝基-L-精氨酸甲酯心脏(IP + L-NAME组,n = 6)在全心缺血20分钟前先进行2分钟缺血预处理,然后在Krebs-Henseleit缓冲液中用3 mmol/L L-NAME再灌注5分钟;缺血预处理加L-精氨酸心脏(IP + ARG组,n = 6)在全心缺血20分钟前先进行2分钟缺血预处理,然后在Krebs-Henseleit缓冲液中用1 mmol/L L-精氨酸再灌注5分钟。连续记录血流动力学参数和冠状动脉流量。在再灌注后5分钟和60分钟测量亚硝酸盐和硝酸盐(NOx),并测定梗死面积。
结果
与GI组、IP组、ARG组和IP + L-NAME组相比,IP + ARG组左心室峰值舒张压和冠状动脉流量有显著改善和保留。与GI组、IP组ARG组和IP + L-NAME组相比,IP + ARG组梗死面积显著减小。与GI组相比,IP + ARG组在再灌注期间观察到NOx有显著保留。
结论
用L-NAME抑制一氧化氮合酶对缺血预处理影响不大,表明内源性NO不是缺血预处理的主要介质。然而,用NO的前体L-精氨酸可增强缺血预处理的效果,改善离体大鼠心脏缺血后的功能恢复和梗死面积。
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