Gene Dosage-Dependent Effects of Cardiac-Specific Overexpression of the A3 Adenosine Receptor

R. Black, Yiru Guo, Z. Ge, S. Murphree, S. Prabhu, W. Jones, R. Bolli, J. Auchampach
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引用次数: 91

Abstract

We used a genetic approach to determine whether increasing the level of A3 adenosine receptors (A3ARs) expressed in the heart confers protection against ischemia without causing cardiac pathology. We generated mice carrying one (A3tg.1) or six (A3tg.6) copies of a transgene consisting of the cardiomyocyte-specific &agr;-myosin heavy chain gene promoter and the A3AR cDNA. A3tg.1 and A3tg.6 mice expressed 12.7±3.15 and 66.3±9.4 fmol/mg of the high-affinity G protein–coupled form of the A3AR in the myocardium, respectively. Extensive morphological, histological, and functional analyses demonstrated that there were no apparent abnormalities in A3tg.1 transgenic mice compared with nontransgenic mice. In contrast, A3tg.6 mice exhibited dilated hearts, expression of markers of hypertrophy, bradycardia, hypotension, and systolic dysfunction. When A3tg mice were subjected to 30 minutes of coronary occlusion and 24 hours of reperfusion, infarct size was reduced ≈30% in A3tg.1 mice and ≈40% in A3tg.6 mice compared with nontransgenic littermates. The reduction in infarct size in the transgenic mice was not related to differences in risk region size, systemic hemodynamics, or body temperature, indicating that the cardioprotection was a result of increased A3AR signaling in the ischemic myocardium. The results demonstrate that low-level expression of A3ARs in the heart provides effective protection against ischemic injury without detectable adverse effects, whereas higher levels of A3AR expression lead to the development of a dilated cardiomyopathy.
A3腺苷受体心脏特异性过表达的基因剂量依赖性效应
我们使用遗传方法来确定增加A3腺苷受体(A3ARs)在心脏中的表达水平是否能在不引起心脏病理的情况下保护心脏免受缺血。我们培养了携带一个(A3tg.1)或六个(A3tg.6)个由心肌细胞特异性&agr;-肌球蛋白重链基因启动子和A3AR cDNA组成的转基因拷贝的小鼠。A3tg。1和A3tg。6只小鼠心肌中分别表达12.7±3.15和66.3±9.4 fmol/mg高亲和G蛋白偶联形式的A3AR。广泛的形态学、组织学和功能分析表明,A3tg没有明显的异常。1转基因小鼠与非转基因小鼠比较。相反,A3tg。6只小鼠表现出心脏扩张,肥厚、心动过缓、低血压和收缩功能障碍标志物的表达。A3tg小鼠冠脉闭塞30分钟,再灌注24小时,A3tg梗死面积减小约30%。在A3tg中约占40%。6只小鼠与非转基因小鼠相比。转基因小鼠梗死面积的减少与危险区大小、全身血流动力学或体温的差异无关,表明心脏保护是缺血心肌中A3AR信号增加的结果。结果表明,心脏中A3AR的低水平表达可有效保护缺血性损伤而无明显的不良反应,而A3AR的高水平表达可导致扩张型心肌病的发展。
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