Timing of adenosine 2A receptor stimulation relative to reperfusion has differential effects on infarct size and cardiac function as assessed in mice by MRI

Zequan Yang; Joel Linden; Stuart S. Berr

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Timing of adenosine 2A receptor stimulation relative to reperfusion has differential effects on infarct size and cardiac function as assessed in mice by MRI

机译：MRI评估小鼠相对于再灌注的腺苷2A受体刺激时机对梗死面积和心功能有不同的影响

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Timing of adenosine 2A receptor stimulation relative to reperfusion has differential effects on infarct size and cardiac function as assessed in mice by MRI. Am J Physiol Heart Circ Phys-iol 295: H2328-H2335, 2008. First published October 10, 2008; doi:10.1152/ajpheart.00091.2008.~he activation of adenosine 2A receptors before reperfusion following coronary artery occlusion reduces infarct size and improves ejection fraction (EF). In this study, we examined the effects of delaying treatment with the adenosine 2A receptor agonist ATL146e (ATL) until 1 h postreperfusion. The infarct size and EF were serially assessed by gadolinium-diethylene-triaminepentaacetic acid-enhanced MRI in C57BL/6 mice at 1 and 24 h postreperfusion. The infarct size was also assessed by 2,3,5-triphenyltetrazolium chloride staining at 24 h. Mice were treated with ATL (10 jJig/kg ip) either 2 min before reperfusion (early ATL) or 1 h postreperfusion (late ATL) following the 45-min coronary occlusion. The two methods used to assess infarct size at 24 h postreperfusion (MRI and 2,3,5-triphenyltetrazolium chloride) showed an excellent correlation (R = 0.96). The risk region, determined at 24 h postreperfusion, was comparable between the control and ATL-treated groups. The infarct size by MRI at 1 versus 24 h postreperfusion was 25 +- 1 vs. 26 +- 1% of left ventricular mass (means +- SE) in control mice, 16 +- 2 versus 17 +- 2% in early-ATL mice, and 24 +- 2 versus 25 +- 2% in late-ATL mice (intragroup, P = not significant; and intergroup, early ATL vs. control or late ATL, P < 0.05). EF was reduced in control mice but was largely preserved between 1 and 24 h in both early-ATL and late-ATL mice (P < 0.05). In conclusion, after coronary occlusion in mice, the extent of myocellular death due to ischemia-reperfusion injury is 95% complete within 1 h of reperfusion. The infarct size was significantly reduced by ATL when given just before reperfusion, but not 1 h postreperfusion. Either treatment window helped preserve the EF between 1 and 24 h postreperfusion

机译：相对于再灌注，腺苷2A受体刺激的时机对梗死面积和心功能有不同的影响，如通过MRI在小鼠中评估的。 Am J Physiol Heart Circ Phys-iol 295：H2328-H2335，2008年。2008年10月10日首次发布; doi：10.1152 / ajpheart.00091.2008。〜冠状动脉闭塞后再灌注前腺苷2A受体的激活减少了梗塞面积并改善了射血分数（EF）。在这项研究中，我们研究了用腺苷2A受体激动剂ATL146e（ATL）延迟治疗直至再灌注后1 h的效果。在再灌注后1小时和24小时，通过g二乙二胺三胺五乙酸增强MRI对C57BL / 6小鼠的梗塞面积和EF进行连续评估。在24小时时，通过2,3,5-三苯基四唑氯化物染色评估梗塞面积。在再灌注前2分钟（早期ATL）或在再灌注后1小时（晚期ATL）45分钟冠状动脉闭塞后，对小鼠进行ATL（10 jJig / kg ip ip）治疗。再灌注后24小时用于评估梗死面积的两种方法（MRI和2,3,5-三苯基四唑鎓氯化物）显示出极好的相关性（R = 0.96）。在再灌注后24小时确定的危险区域在对照组和ATL治疗组之间是可比较的。 MRI在再灌注后1小时和24小时时的梗死面积为对照组小鼠左心室质量的25 +1对26％-1％（平均值+ SE），早期小鼠为16 +/- 2对17 + 2％。 ATL小鼠，晚期ATL小鼠为24±2，而25±2％（组内，P =不显着;组间，早期ATL与对照组或晚期ATL，P <0.05）。对照小鼠的EF降低，但在早期ATL和晚期ATL小鼠中EF大部分都保留了1至24 h（P <0.05）。总之，在小鼠冠状动脉闭塞后，缺血再灌注损伤引起的心肌细胞死亡程度在再灌注后1小时内完成了95％。在再灌注前给予ATL可以显着减少梗死面积，而在再灌注后1 h则不能。任一治疗窗口均有助于在再灌注后1至24小时内保持EF

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《American Journal of Physiology》 |2009年第2期|共8页
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Zequan Yang; Joel Linden; Stuart S. Berr;
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1. Timing of adenosine 2A receptor stimulation relative to reperfusion has differential effects on infarct size and cardiac function as assessed in mice by MRI [J] . Zequan Yang, Joel Linden, Stuart S. Berr American Journal of Physiology . 2009,第6aPta2期

机译：MRI评估小鼠相对于再灌注的腺苷2A受体刺激时机对梗死面积和心功能有不同的影响
2. Timing of adenosine 2A receptor stimulation relative to reperfusion has differential effects on infarct size and cardiac function as assessed in mice by MRI [J] . Zequan Yang, Joel Linden, Stuart S. Berr American Journal of Physiology . 2008,第6aPta2期

机译：相对于再灌注的腺苷2a受体刺激的时序对MICE中的小鼠评估的梗塞大小和心脏功能具有差异效应
3. Timing of adenosine 2A receptor stimulation relative to reperfusion has differential effects on infarct size and cardiac function as assessed in mice by MRI [J] . Zequan Yang, Joel Linden, Stuart S. Berr American Journal of Physiology . 2008,第6aPta2期

机译：MRI评估小鼠相对于再灌注的腺苷2A受体刺激时机对梗死面积和心功能有不同的影响
4. Cardiac specific iNOS-overexpression in transgenic mice antagonizes the cardiac effects of beta-adrenergic stimulation in vivo [C] . A. Molojavyi, C. Jacoby, J. Heger, Nordrhein-Westfa?lische Akademie der Wissenschaften . 2005

机译：转基因小鼠中的心脏特异性Inos-过表达拮抗体内β-肾上腺素能刺激的心脏作用
5. The cardiovascular effects of CGS 21680, an adenosine A(2A) receptor agonist and 17beta-estradiol in rats with impaired cardiac function. [D] . Nekooeian, Ali Akbar. 1999

机译：CGS 21680，腺苷A（2A）受体激动剂和17β-雌二醇对心脏功能受损的大鼠的心血管作用。
6. Timing of adenosine 2A receptor stimulation relative to reperfusion has differential effects on infarct size and cardiac function as assessed in mice by MRI [O] . Zequan Yang, Joel Linden, Stuart S. Berr, -1

机译：MRI评估小鼠相对于再灌注的腺苷2A受体刺激时机对梗死面积和心功能有不同的影响
7. Timing of adenosine 2A receptor stimulation relative to reperfusion has differential effects on infarct size and cardiac function as assessed in mice by MRI [O] . Yang, Zequan, Linden, Joel, Berr, Stuart S., 2008

机译：MRI评估小鼠相对于再灌注的腺苷2A受体刺激时机对梗死面积和心功能有不同的影响

Timing of adenosine 2A receptor stimulation relative to reperfusion has differential effects on infarct size and cardiac function as assessed in mice by MRI

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