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nArgBP2-SAPAP-SHANK,与精神疾病相关的核心突触后三联体。

nArgBP2-SAPAP-SHANK, the core postsynaptic triad associated with psychiatric disorders.

机构信息

Department of Physiology and Biomedical Sciences, Seoul National University College of Medicine, Seoul, 03080, South Korea.

Interdisciplinary Program in Neuroscience, College of Natural Sciences, Seoul National University, Seoul, 08826, South Korea.

出版信息

Exp Mol Med. 2018 Apr 9;50(4):1-9. doi: 10.1038/s12276-017-0018-5.

Abstract

Despite the complex genetic architecture, a broad spectrum of psychiatric disorders can still be caused by mutation(s) in the same gene. These disorders are interrelated with overlapping causative mechanisms including variations in the interaction among the risk-associated proteins that may give rise to the specific spectrum of each disorder. Additionally, multiple lines of evidence implicate an imbalance between excitatory and inhibitory neuronal activity (E/I imbalance) as the shared key etiology. Thus, understanding the molecular mechanisms underlying E/I imbalance provides essential insight into the etiology of these disorders. One important class of candidate risk genes is the postsynaptic scaffolding proteins, such as nArgBP2, SAPAP, and SHANK that regulate the actin cytoskeleton in dendritic spines of excitatory synapses. This review will cover and discuss recent studies that examined how these proteins, especially nArgBP2, are associated with psychiatric disorders. Next, we propose a possibility that variations in the interaction among these proteins in a specific brain region might contribute to the onset of diverse phenotypes of psychiatric disorders.

摘要

尽管遗传结构复杂,但许多精神疾病仍可能是由同一基因中的突变引起的。这些疾病相互关联,其致病机制重叠,包括风险相关蛋白相互作用的变化,这些变化可能导致每种疾病的特定表现。此外,多条证据表明兴奋性和抑制性神经元活动之间的不平衡(E/I 失衡)是共同的关键病因。因此,了解 E/I 失衡的分子机制为这些疾病的病因提供了重要的见解。候选风险基因的一个重要类别是突触后支架蛋白,如 nArgBP2、SAPAP 和 SHANK,它们调节兴奋性突触树突棘中的肌动蛋白细胞骨架。本综述将涵盖和讨论最近的研究,这些研究检查了这些蛋白,特别是 nArgBP2,如何与精神疾病相关。接下来,我们提出一种可能性,即在特定脑区这些蛋白之间相互作用的变化可能导致精神疾病不同表型的发生。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cb5e/5938024/54bc9d83d99f/12276_2017_18_Fig1_HTML.jpg

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