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Multifunctional role of astrocytes as gatekeepers of neuronal energy supply

机译:星形胶质细胞在神经元能量供应中的多功能作用

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摘要

Dynamic adjustments to neuronal energy supply in response to synaptic activity are critical for neuronal function. Glial cells known as astrocytes have processes that ensheath most central synapses and express G-protein-coupled neurotransmitter receptors and transporters that respond to neuronal activity. Astrocytes also release substrates for neuronal oxidative phosphorylation and have processes that terminate on the surface of brain arterioles and can influence vascular smooth muscle tone and local blood flow. Membrane receptor or transporter-mediated effects of glutamate represent a convergence point of astrocyte influence on neuronal bioenergetics. Astrocytic glutamate uptake drives glycolysis and subsequent shuttling of lactate from astrocytes to neurons for oxidative metabolism. Astrocytes also convert synaptically reclaimed glutamate to glutamine, which is returned to neurons for glutamate salvage or oxidation. Finally, astrocytes store brain energy currency in the form of glycogen, which can be mobilized to produce lactate for neuronal oxidative phosphorylation in response to glutamatergic neurotransmission. These mechanisms couple synaptically driven astrocytic responses to glutamate with release of energy substrates back to neurons to match demand with supply. In addition, astrocytes directly influence the tone of penetrating brain arterioles in response to glutamatergic neurotransmission, coordinating dynamic regulation of local blood flow. We will describe the role of astrocytes in neurometabolic and neurovascular coupling in detail and discuss, in turn, how astrocyte dysfunction may contribute to neuronal bioenergetic deficit and neurodegeneration. Understanding the role of astrocytes as a hub for neurometabolic and neurovascular coupling mechanisms is a critical underpinning for therapeutic development in a broad range of neurodegenerative disorders characterized by chronic generalized brain ischemia and brain microvascular dysfunction.
机译:响应突触活动对神经元能量供应的动态调节对于神经元功能至关重要。称为星形胶质细胞的神经胶质细胞具有包裹大多数中枢突触的过程,并表达对神经元活动起反应的G蛋白偶联神经递质受体和转运蛋白。星形胶质细胞还释放神经元氧化磷酸化的底物,并具有终止于脑小动脉表面的过程,并可影响血管平滑肌张力和局部血流。谷氨酸的膜受体或转运蛋白介导的作用代表星形胶质细胞对神经元生物能学影响的收敛点。星形胶质细胞谷氨酸的摄取驱动糖酵解,随后乳酸从星形胶质细胞穿梭到神经元进行氧化代谢。星形胶质细胞还将突触回收的谷氨酸转化为谷氨酰胺,谷氨酰胺返回到神经元以进行谷氨酸的拯救或氧化。最后,星形胶质细胞以糖原的形式储存脑能量,可以响应谷氨酸能神经传递而动员产生乳酸以进行神经元氧化磷酸化。这些机制将对谷氨酸的突触驱动的星形细胞反应与能量底物释放回到神经元耦合,以使需求与供应相匹配。此外,星形胶质细胞直接响应谷氨酸能神经传递而影响穿透性脑小动脉的音调,从而协调局部血流的动态调节。我们将详细描述星形胶质细胞在神经代谢和神经血管偶联中的作用,并依次讨论星形胶质细胞功能障碍如何导致神经元生物能缺乏和神经退行性变。了解星形胶质细胞作为神经代谢和神经血管偶联机制的枢纽的作用,对于以慢性全身性脑缺血和脑微血管功能障碍为特征的多种神经退行性疾病的治疗发展至关重要。

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