A3 腺苷受体的靶向缺失赋予对心肌缺血损伤的抗性,且不阻止早期预处理。
Targeted deletion of the A3 adenosine receptor confers resistance to myocardial ischemic injury and does not prevent early preconditioning.
作者信息
Guo Y, Bolli R, Bao W, Wu W J, Black R G, Murphree S S, Salvatore C A, Jacobson M A, Auchampach J A
机构信息
Division of Cardiology, University of Louisville and Jewish Heart and Lung Institute, Louisville, Kentucky 40202, USA.
出版信息
J Mol Cell Cardiol. 2001 Apr;33(4):825-30. doi: 10.1006/jmcc.2001.1338.
Abstract
We used mice with genetic disruption of the A3 adenosine receptor (AR) gene (A3AR(-/-)mice) to assess the in vivo role of the A3AR in modulating myocardial ischemia/reperfusion injury and preconditioning (PC). Surprisingly, infarct size induced by 30 min of coronary artery occlusion and 24 h of reperfusion was 35% smaller in A3AR(-/-)compared to wild-type mice (A3AR(+/+)). The reduction in infarct size was not the result of differences in heart rate, body temperature or increased cardiac expression of A1ARs. However, neutrophil infiltration within infarcted regions was less in A3AR(-/-)mice. Furthermore, ischemic PC induced by either a single episode (one 5 min occlusion) or multiple episodes (six 4 min occlusions) of ischemia produced equivalent reductions in infarct size in A3AR(-/-)and A3AR(+/+)mice. These results indicate that, in the mouse, (i) A3ARs play an injurious role during acute myocardial ischemia/reperfusion injury, possibly by exacerbating the inflammatory response, and (ii) A3ARs are not necessary for the development of the early phase of ischemic PC.
摘要
我们使用A3腺苷受体(AR)基因发生遗传破坏的小鼠(A3AR(-/-)小鼠)来评估A3AR在调节心肌缺血/再灌注损伤及预处理(PC)中的体内作用。令人惊讶的是,与野生型小鼠(A3AR(+/+))相比,A3AR(-/-)小鼠在冠状动脉闭塞30分钟及再灌注24小时后诱导产生的梗死面积小35%。梗死面积的减小并非心率、体温差异或心脏A1AR表达增加所致。然而,A3AR(-/-)小鼠梗死区域内的中性粒细胞浸润较少。此外,单次缺血发作(一次5分钟闭塞)或多次缺血发作(六次4分钟闭塞)诱导的缺血预处理在A3AR(-/-)和A3AR(+/+)小鼠中产生的梗死面积减小程度相当。这些结果表明,在小鼠中,(i)A3AR在急性心肌缺血/再灌注损伤期间发挥有害作用,可能是通过加剧炎症反应,以及(ii)A3AR对于缺血预处理早期阶段的发展并非必需。
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