精神疾病中线粒体遗传学和线粒体通路的复杂相互作用。

Molecular Neuropsychiatry Pub Date : 2018-06-01 Epub Date: 2018-05-30 DOI:10.1159/000488031
Ari B Cuperfain, Zhi Lun Zhang, James L Kennedy, Vanessa F Gonçalves
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引用次数: 45

摘要

虽然大脑只占身体重量的2%,但它却消耗了身体总能量的20%。毫不奇怪,代谢功能障碍和能量供需不匹配与各种神经和精神疾病有关。线粒体负责为大脑提供大部分的能量需求,而大脑将葡萄糖作为其唯一的能量来源。探索线粒体功能障碍在精神疾病病因学中的作用是进一步研究的有希望的途径。线粒体活性的遗传分析是理解与代谢功能障碍相关的疾病发病机制的基础。与神经影像学和病理研究相一致,遗传学在精神疾病的生化发现和临床相关性之间提供了一个重要的桥梁。线粒体遗传学的分析有几个独特的方面,以及相应的特殊考虑。在这里,我们回顾了线粒体遗传分析的组成部分——核DNA、线粒体DNA、线粒体途径、假基因、核线粒体错配和microrna——这些可能有助于观察到的临床表型。在整个过程中,我们强调了由于这些过程的功能障碍而可能引起的精神疾病,重点是精神分裂症和双相情感障碍。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The Complex Interaction of Mitochondrial Genetics and Mitochondrial Pathways in Psychiatric Disease.

The Complex Interaction of Mitochondrial Genetics and Mitochondrial Pathways in Psychiatric Disease.

The Complex Interaction of Mitochondrial Genetics and Mitochondrial Pathways in Psychiatric Disease.

The Complex Interaction of Mitochondrial Genetics and Mitochondrial Pathways in Psychiatric Disease.

While accounting for only 2% of the body's weight, the brain utilizes up to 20% of the body's total energy. Not surprisingly, metabolic dysfunction and energy supply-and-demand mismatch have been implicated in a variety of neurological and psychiatric disorders. Mitochondria are responsible for providing the brain with most of its energetic demands, and the brain uses glucose as its exclusive energy source. Exploring the role of mitochondrial dysfunction in the etiology of psychiatric disease is a promising avenue to investigate further. Genetic analysis of mitochondrial activity is a cornerstone in understanding disease pathogenesis related to metabolic dysfunction. In concert with neuroimaging and pathological study, genetics provides an important bridge between biochemical findings and clinical correlates in psychiatric disease. Mitochondrial genetics has several unique aspects to its analysis, and corresponding special considerations. Here, we review the components of mitochondrial genetic analysis - nuclear DNA, mitochon-drial DNA, mitochondrial pathways, pseudogenes, nuclear-mitochondrial mismatch, and microRNAs - that could contribute to an observable clinical phenotype. Throughout, we highlight psychiatric diseases that can arise due to dysfunction in these processes, with a focus on schizophrenia and bipolar disorder.

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