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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Metabolic alterations induced by ischemia in primary cultures of astrocytes: merging ~(13)C NMR spectroscopy and metabolic flux analysis
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Metabolic alterations induced by ischemia in primary cultures of astrocytes: merging ~(13)C NMR spectroscopy and metabolic flux analysis

机译:星形胶质细胞原代培养中缺血引起的代谢变化:〜(13)C NMR光谱和代谢通量分析的合并

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摘要

Disruption of brain energy metabolism is the hallmark of cerebral ischemia, a major cause of death worldwide. Astrocytes play a key role in the regulation of brain metabolism and their vulnerability to ischemia has been described. Aiming to quantify the effects of an ischemic insult in astrocytic metabolism, primary cultures of astrocytes were subjected to 5 h of oxygen and glucose deprivation in a bioreactor. Flux distributions, before and after ischemia, were estimated by metabolic flux analysis using isotopic information and the consumption/secretion rates of relevant extracellular metabolites as constraints. During ischemia and early recovery, 30% of cell death was observed; several metabolic alterations were also identified reflecting a metabolic response by the surviving cells. In the early recovery (approx10 h), astrocytes up-regulated glucose utilization by 30% and increased the pentose phosphate pathway and tricarboxylic acid cycle fluxes by three and twofold, respectively. Additionally, a two to fivefold enhancement in branched-chain amino acids catabolism suggested the importance of anaplerotic molecules to the fast recovery of the energetic state, which was corroborated by measured cellular ATP levels. Glycolytic metabolism was predominant in the late recovery. In summary, this work demonstrates that changes in fluxes of key metabolic pathways are implicated in the recovery from ischemia in astrocytes.
机译:脑能量代谢的中断是脑缺血的标志,脑缺血是全球范围内的主要死亡原因。星形胶质细胞在调节脑代谢中起关键作用,并且已经描述了它们对缺血的脆弱性。为了量化缺血性损伤对星形细胞代谢的影响,星形胶质细胞的原代培养物在生物反应器中经历了5 h的氧气和葡萄糖剥夺。通过代谢通量分析,使用同位素信息和相关细胞外代谢物的消耗/分泌速率作为约束条件,估计缺血前后的通量分布。在缺血和早期恢复过程中,观察到30%的细胞死亡。还确定了几种代谢改变,反映了存活细胞的代谢反应。在早期恢复期(约10小时),星形胶质细胞上调葡萄糖利用率30%,并使戊糖磷酸途径和三羧酸循环通量分别增加三倍和两倍。此外,支链氨基酸分解代谢提高了2到5倍,这表明过失分子对于快速恢复精力旺盛状态的重要性,这一点已通过测量的细胞ATP水平得到证实。糖酵解代谢在恢复后期占主导地位。总而言之,这项工作表明,关键代谢途径通量的变化与星形胶质细胞缺血的恢复有关。

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