Spontaneous Ischemic Events in the Brain and Heart Adapt the Hearts of Severely Atherosclerotic Mice to Ischemia

S. Tokuno, K. Hinokiyama, K. Tokuno, C. Löwbeer, L. Hansson, G. Valen
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引用次数: 61

Abstract

To investigate if spontaneous ischemic events in mice with severe multi-organ atherosclerosis could adapt to ischemia, apolipoprotein E/LDL receptor knockout mice were fed an atherogenic diet for 7 to 9 months. Signs of spontaneous ischemia occurred. One to two days later, hearts were excised, Langendorff-perfused with induced global ischemia, and compared with mice without signs of disease. In vivo heart or brain infarctions were verified by heart histology and/or increased serum levels of cardiac troponin T and S100B. Hearts of mice with spontaneous ischemic events had improved function and reduced Langendorff-induced infarctions. To investigate the remote preconditioning effect of brain ischemia, bilateral ligation of the internal carotid arteries was performed in C57BL6 mice. Twenty-four hours later, their isolated hearts were protected against induced global ischemia. A possible role of inducible NO synthase (iNOS) was studied in iNOS knock out mice, who were not preconditioned by induced brain ischemia. Cardiac iNOS was unchanged 24 hours after preconditioning, suggesting that NO is a trigger rather than a mediator of protection. These findings suggest that spontaneous ischemic events in the brain and heart adapt the heart to ischemia. This can be mimicked by induced brain ischemia, with iNOS as a key factor of protection.
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脑和心脏的自发缺血事件使严重动脉粥样硬化小鼠的心脏适应缺血
为了研究严重多器官动脉粥样硬化小鼠自发性缺血事件是否能适应缺血,我们给载脂蛋白E/LDL受体敲除小鼠喂食致动脉粥样硬化饮食7 ~ 9个月。出现自发性缺血的迹象。一到两天后,切除心脏,用langendorff灌注诱导的全脑缺血,并与没有疾病迹象的小鼠进行比较。通过心脏组织学和/或心肌肌钙蛋白T和S100B升高的血清水平来验证体内心脏或脑梗死。自发性缺血事件小鼠的心脏功能得到改善,langendorff诱导的梗死减少。为了研究脑缺血的远程预处理作用,我们对C57BL6小鼠进行了双侧颈内动脉结扎。24小时后,他们的离体心脏受到保护,免受诱导的全身缺血。研究了诱导型NO合成酶(iNOS)在未进行脑缺血预处理的iNOS敲除小鼠中的可能作用。预处理后24小时心肌iNOS未发生变化,提示NO是一种触发因子而非保护介质。这些发现表明,大脑和心脏的自发缺血事件使心脏适应缺血。这可以通过诱导脑缺血来模拟,其中iNOS是一个关键的保护因子。
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