首页> 外文期刊>Journal of Cerebral Blood Flow and Metabolism: Official Journal of the International Society of Cerebral Blood Flow and Metabolism >Selective cerebral perfusion prevents abnormalities in glutamate cycling and neuronal apoptosis in a model of infant deep hypothermic circulatory arrest and reperfusion
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Selective cerebral perfusion prevents abnormalities in glutamate cycling and neuronal apoptosis in a model of infant deep hypothermic circulatory arrest and reperfusion

机译:选择性脑灌注可防止婴儿深低温循环性停搏和再灌注模型中的谷氨酸循环异常和神经元凋亡

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Deep hypothermic circulatory arrest is often required for the repair of complex congenital cardiac defects in infants. However, deep hypothermic circulatory arrest induces neuroapoptosis associated with later development of neurocognitive abnormalities. Selective cerebral perfusion theoretically provides superior neural protection possibly through modifications in cerebral substrate oxidation and closely integrated glutamate cycling. We tested the hypothesis that selective cerebral perfusion modulates glucose utilization, and ameliorates abnormalities in glutamate flux, which occur in association with neuroapoptosis during deep hypothermic circulatory arrest. Eighteen infant male Yorkshire piglets were assigned randomly to two groups of seven (deep hypothermic circulatory arrest or deep hypothermic circulatory arrest with selective cerebral perfusion for 60 minutes at 18?) and four control pigs without cardiopulmonary bypass support. Carbon-13-labeled glucose as a metabolic tracer was infused, and gas chromatography-mass spectrometry and nuclear magnetic resonance were used for metabolic analysis in the frontal cortex. Following 2.5h of cerebral reperfusion, we observed similar cerebral adenosine triphosphate levels, absolute levels of lactate and citric acid cycle intermediates, and carbon-13 enrichment among three groups. However, deep hypothermic circulatory arrest induced significant abnormalities in glutamate cycling resulting in reduced glutamate/glutamine and elevated -aminobutyric acid/glutamate along with neuroapoptosis, which were all prevented by selective cerebral perfusion. The data suggest that selective cerebral perfusion prevents these modifications in glutamate/glutamine/-aminobutyric acid cycling and protects the cerebral cortex from apoptosis.
机译:通常需要深低温热循环停止来修复婴儿复杂的先天性心脏缺陷。但是,深部低温循环停止会诱导神经凋亡,并与后来出现的神经认知异常有关。理论上,选择性脑灌注可能通过修饰脑底物氧化和紧密整合的谷氨酸循环来提供卓越的神经保护作用。我们测试了选择性脑灌注调节葡萄糖利用并改善谷氨酸通量异常的假说,谷氨酸通量异常是在深低温循环停止期间与神经细胞凋亡相关的。 18只婴儿约克郡雄性仔猪被随机分为两组,每组七只(深低温循环停滞或深低温循环停滞,在18℃选择性脑灌注60分钟),另外四只则没有体外循环支持。注入了碳13标记的葡萄糖作为代谢示踪剂,并使用了气相色谱-质谱和核磁共振技术对额叶皮层进行了代谢分析。在脑再灌注2.5小时后,我们观察到三组脑相似的三磷酸腺苷水平,乳酸和柠檬酸循环中间体的绝对水平以及碳13富集。然而,深低温循环停止导致谷氨酸循环明显异常,导致谷氨酸/谷氨酰胺减少和-氨基丁酸/谷氨酸升高以及神经细胞凋亡,所有这些都可以通过选择性脑灌注来预防。数据表明选择性脑灌注可防止谷氨酸/谷氨酰胺/-氨基丁酸循环中的这些修饰,并保护大脑皮层免于凋亡。

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