谷氨酸-谷氨酰胺神经递质循环模型。

Frontiers in neuroenergetics Pub Date : 2013-01-28 eCollection Date: 2013-01-01 DOI:10.3389/fnene.2013.00001
Jun Shen
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引用次数: 72

摘要

谷氨酸是大脑中主要的兴奋性神经递质。虽然谷氨酸在神经组织中由葡萄糖快速合成,但谷氨酸释放后补充神经递质谷氨酸的生化过程涉及谷氨酸-谷氨酰胺循环。自1994年以来,不同实验室进行的大量体内(13)C磁共振波谱(MRS)实验一致得出结论:(1)谷氨酸-谷氨酰胺循环是一种主要的代谢途径,其通量率大大高于早期细胞培养和脑切片研究表明的通量率;(2)谷氨酸-谷氨酰胺循环与脑功能总能量需求的很大一部分相耦合。谷氨酸作为中枢神经系统的主要神经递质和连接碳氮代谢的关键代谢物的双重作用,使得利用MRS测量谷氨酸和谷氨酰胺的标记动力学来探测谷氨酸神经递质循环成为可能。同时,与非氨基酸神经递质相比,增加的复杂性使得从代谢中定量分离神经传递事件更具挑战性。在过去的几年里,我们对谷氨酸-谷氨酰胺循环的神经元-星形胶质双室代谢模型的理解有了很大的进展。特别是,谷氨酰胺同位素稀释在使用[1-(13)C]或[1,6-(13)C(2)]葡萄糖测定谷氨酸-谷氨酰胺循环速率方面的重要性已被不同的实验室证明和再现。本文综述了谷氨酸-谷氨酰胺循环双室模型的最新进展。特别地,分析了谷氨酰胺同位素稀释对测定谷氨酸-谷氨酰胺循环速率的各种标记策略的影响。本文还提出了对谷氨酰胺同位素稀释不敏感的谷氨酸-谷氨酰胺循环通量测量的实验策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Modeling the glutamate-glutamine neurotransmitter cycle.

Glutamate is the principal excitatory neurotransmitter in brain. Although it is rapidly synthesized from glucose in neural tissues the biochemical processes for replenishing the neurotransmitter glutamate after glutamate release involve the glutamate-glutamine cycle. Numerous in vivo(13)C magnetic resonance spectroscopy (MRS) experiments since 1994 by different laboratories have consistently concluded: (1) the glutamate-glutamine cycle is a major metabolic pathway with a flux rate substantially greater than those suggested by early studies of cell cultures and brain slices; (2) the glutamate-glutamine cycle is coupled to a large portion of the total energy demand of brain function. The dual roles of glutamate as the principal neurotransmitter in the CNS and as a key metabolite linking carbon and nitrogen metabolism make it possible to probe glutamate neurotransmitter cycling using MRS by measuring the labeling kinetics of glutamate and glutamine. At the same time, comparing to non-amino acid neurotransmitters, the added complexity makes it more challenging to quantitatively separate neurotransmission events from metabolism. Over the past few years our understanding of the neuronal-astroglial two-compartment metabolic model of the glutamate-glutamine cycle has been greatly advanced. In particular, the importance of isotopic dilution of glutamine in determining the glutamate-glutamine cycling rate using [1-(13)C] or [1,6-(13)C(2)] glucose has been demonstrated and reproduced by different laboratories. In this article, recent developments in the two-compartment modeling of the glutamate-glutamine cycle are reviewed. In particular, the effects of isotopic dilution of glutamine on various labeling strategies for determining the glutamate-glutamine cycling rate are analyzed. Experimental strategies for measuring the glutamate-glutamine cycling flux that are insensitive to isotopic dilution of glutamine are also suggested.

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