Brain network and energy imbalance in Parkinson's disease: linking ATP reduction and α-synuclein pathology.

IF 3.5 3区医学 Q2 NEUROSCIENCES

Frontiers in Molecular Neuroscience Pub Date : 2025-01-22 eCollection Date: 2024-01-01 DOI:10.3389/fnmol.2024.1507033

Hirohisa Watanabe, Sayuri Shima, Kazuya Kawabata, Yasuaki Mizutani, Akihiro Ueda, Mizuki Ito

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引用次数: 0

Abstract

Parkinson's disease (PD) involves the disruption of brain energy homeostasis. This encompasses broad-impact factors such as mitochondrial dysfunction, impaired glycolysis, and other metabolic disturbances, like disruptions in the pentose phosphate pathway and purine metabolism. Cortical hubs, which are highly connected regions essential for coordinating multiple brain functions, require significant energy due to their dense synaptic activity and long-range connections. Deficits in ATP production in PD can severely impair these hubs. The energy imbalance also affects subcortical regions, including the massive axonal arbors in the striatum of substantia nigra pars compacta neurons, due to their high metabolic demand. This ATP decline may result in α-synuclein accumulation, autophagy-lysosomal system impairment, neuronal network breakdown and accelerated neurodegeneration. We propose an "ATP Supply-Demand Mismatch Model" to help explain the pathogenesis of PD. This model emphasizes how ATP deficits drive pathological protein aggregation, impaired autophagy, and the degeneration of key brain networks, contributing to both motor and non-motor symptoms.

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帕金森病的脑网络和能量失衡：ATP减少与α-突触核蛋白病理的联系

帕金森病（PD）涉及大脑能量稳态的破坏。这包括影响广泛的因素，如线粒体功能障碍、糖酵解受损和其他代谢紊乱，如戊糖磷酸途径和嘌呤代谢的中断。皮质中枢是高度连接的区域，对协调多种脑功能至关重要，由于其密集的突触活动和远程连接，需要大量的能量。PD中ATP产生的缺陷会严重损害这些中枢。能量失衡还影响皮质下区域，包括黑质致密部神经元纹状体的大量轴突乔木，由于它们的高代谢需求。这种ATP下降可能导致α-突触核蛋白积累，自噬-溶酶体系统损伤，神经网络破坏和神经退行性变加速。我们提出了一个“ATP供需不匹配模型”来帮助解释帕金森病的发病机制。该模型强调ATP缺陷如何驱动病理性蛋白质聚集、自噬受损和关键脑网络退化，从而导致运动和非运动症状。

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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来源期刊

Frontiers in Molecular Neuroscience NEUROSCIENCES-

CiteScore

5.70

自引率

2.10%

发文量

669

审稿时长

14 weeks

期刊介绍： Frontiers in Molecular Neuroscience is a first-tier electronic journal devoted to identifying key molecules, as well as their functions and interactions, that underlie the structure, design and function of the brain across all levels. The scope of our journal encompasses synaptic and cellular proteins, coding and non-coding RNA, and molecular mechanisms regulating cellular and dendritic RNA translation. In recent years, a plethora of new cellular and synaptic players have been identified from reduced systems, such as neuronal cultures, but the relevance of these molecules in terms of cellular and synaptic function and plasticity in the living brain and its circuits has not been validated. The effects of spine growth and density observed using gene products identified from in vitro work are frequently not reproduced in vivo. Our journal is particularly interested in studies on genetically engineered model organisms (C. elegans, Drosophila, mouse), in which alterations in key molecules underlying cellular and synaptic function and plasticity produce defined anatomical, physiological and behavioral changes. In the mouse, genetic alterations limited to particular neural circuits (olfactory bulb, motor cortex, cortical layers, hippocampal subfields, cerebellum), preferably regulated in time and on demand, are of special interest, as they sidestep potential compensatory developmental effects.