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首页> 外文期刊>The Journal of Thoracic and Cardiovascular Surgery >Adenosine-enhanced ischemic preconditioning provides enhanced postischemic recovery and limitation of infarct size in the rabbit heart.
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Adenosine-enhanced ischemic preconditioning provides enhanced postischemic recovery and limitation of infarct size in the rabbit heart.

机译:腺苷增强的缺血预处理可增强缺血后恢复能力,并限制兔心脏梗死面积。

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摘要

OBJECTIVE: The purpose of this study was to determine the effect of an intracoronary bolus injection of adenosine used in concert with ischemic preconditioning on postischemic functional recovery and infarct size reduction in the rabbit heart and to compare adenosine-enhanced ischemic preconditioning with ischemic preconditioning and magnesium-supplemented potassium cardioplegia. METHODS: New Zealand White rabbits (n = 36) were used for Langendorff perfusion. Control hearts were perfused at 37 degrees C for 180 minutes; global ischemic hearts received 30 minutes of global ischemia and 120 minutes of reperfusion; magnesium-supplemented potassium cardioplegic hearts received cardioplegia 5 minutes before global ischemia; ischemic preconditioned hearts received 5 minutes of zero-flow global ischemia and 5 minutes of reperfusion before global ischemia; adenosine-enhanced ischemic preconditioned hearts received a bolus injection of adenosine just before the preconditioning. To separate the effects of adenosine from adenosine-enhanced ischemic preconditioning, a control group received a bolus injection of adenosine 10 minutes before global ischemia. RESULTS: Infarct volume in global ischemic hearts was 32.9% +/- 5.1% and 1.03% +/- 0.3% in control hearts. The infarct volume decreased (10.23% +/- 2.6% and 7.0% +/- 1.6%, respectively; p < 0.001 versus global ischemia) in the ischemic preconditioned group and control group, but this did not enhance postischemic functional recovery. Magnesium-supplemented potassium cardioplegia and adenosine-enhanced ischemic preconditioning significantly decreased infarct volume (2.9% +/- 0.8% and 2.8% +/- 0.55%, respectively; p < 0.001 versus global ischemia, p = 0.02 versus ischemic preconditioning and p = 0.05 versus control group) and significantly enhanced postischemic functional recovery. CONCLUSIONS: Adenosine-enhanced ischemic preconditioning is superior to ischemic preconditioning and provides equal protection to that afforded by magnesium-supplemented potassium cardioplegia.
机译:目的:本研究旨在确定冠状动脉内注射腺苷与缺血预处理相结合对兔心脏缺血后功能恢复和梗死面积缩小的影响,并比较腺苷增强缺血预处理与镁预处理和镁的比较-补充钾心脏停搏。方法:将新西兰白兔(n = 36)用于Langendorff灌注。对照心脏在37摄氏度下灌注180分钟;全球缺血性心脏接受了30分钟的全局缺血和120分钟的再灌注;镁补充的钾心脏停搏心脏在整体缺血前5分钟接受了心脏停搏;缺血预处理的心脏在整体缺血前接受了5分钟的零流量全局缺血和5分钟的再灌注;腺苷增强的缺血性预处理心脏在预处理之前就接受了大剂量腺苷的快速浓注。为了从腺苷增强的缺血预处理中分离出腺苷的作用,对照组在整体缺血前10分钟接受了大剂量的腺苷推注。结果:整体缺血心脏的梗死体积为32.9%+/- 5.1%,对照心脏为1.03%+/- 0.3%。在缺血预处理组和对照组中,梗塞体积减少(分别为10.23%+ /-2.6%和7.0%+ /-1.6%;与整体缺血相比,p <0.001),但这并没有增强缺血后功能的恢复。镁补充的钾心脏停搏和腺苷增强的缺血预处理显着降低了梗塞体积(分别为2.9%+/- 0.8%和2.8%+/- 0.55%;相对于整体缺血,p <0.001,相对于缺血预处理的p = 0.02,和=与对照组相比为0.05),并显着增强了缺血后功能恢复。结论:腺苷增强的缺血预适应优于缺血预适应,并提供与镁补充的钾心脏停搏所提供的相同的保护。

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