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一氧化氮合酶1适配蛋白(NOS1AP)在神经和精神疾病中的研究进展

Research progress in NOS1AP in neurological and psychiatric diseases.

作者信息

Wang Jie, Jin Lei, Zhu Yufu, Zhou Xiuping, Yu Rutong, Gao Shangfeng

机构信息

The Graduate School, Xuzhou Medical College, 209 Tong-Shan Road, Xuzhou, 221004, Jiangsu, People's Republic of China.

Brain Hospital, Affiliated Hospital of Xuzhou Medical College, 99 West Huai-Hai Road, Xuzhou 221002, Jiangsu, People's Republic of China.

出版信息

Brain Res Bull. 2016 Jul;125:99-105. doi: 10.1016/j.brainresbull.2016.05.014. Epub 2016 May 26.

DOI:10.1016/j.brainresbull.2016.05.014
PMID:27237129
Abstract

Nitric Oxide Synthase 1 Adaptor Protein (NOS1AP, previously named CAPON) was firstly identified in rat brain in 1998. Structurally, NOS1AP consists of a phosphotyrosine-binding (PTB) domain at its N-terminal and a PDZ (PSD-95/discs-large/ZO-1) ligand motif at its C-terminal. The PTB domain of NOS1AP mediates the interactions with Dexras1, scribble, and synapsins. The PDZ ligand motif of NOS1AP binds to the PDZ domain of NOS1, the enzyme responsible for nitric oxide synthesis in the nervous system. NOS1AP is implicated in Dexras1 activation, neuronal nitric oxide production, Hippo pathway signaling, and dendritic development through the association with these important partners. An increasing body of evidence is pointing to the significant roles of NOS1AP in excitotoxic neuronal damage, traumatic nervous system injury, bipolar disorder, and schizophrenia. However, the study progress in NOS1AP in neurological or psychiatric diseases, has not been systematically reviewed. Here we introduce the expression, structure, and isoforms of NOS1AP, then summarize the physiological roles of NOS1AP, and discuss the relationships between NOS1AP alterations and the pathophysiology of some neurological and psychiatric disorders. The review will promote the further investigation of NOS1AP in brain disorders and the development of drugs targeting the NOS1AP PTB domain or PDZ-binding motif in the future.

摘要

一氧化氮合酶1衔接蛋白(NOS1AP,以前称为CAPON)于1998年首次在大鼠脑中被鉴定出来。在结构上,NOS1AP在其N端由一个磷酸酪氨酸结合(PTB)结构域和在其C端由一个PDZ(PSD-95/盘状大蛋白/ZO-1)配体基序组成。NOS1AP的PTB结构域介导与Dexras1、scribble和突触素的相互作用。NOS1AP的PDZ配体基序与NOS1的PDZ结构域结合,NOS1是负责神经系统中一氧化氮合成的酶。通过与这些重要伙伴的关联,NOS1AP参与Dexras1激活、神经元一氧化氮产生、Hippo信号通路以及树突发育。越来越多的证据表明NOS1AP在兴奋性毒性神经元损伤、创伤性神经系统损伤、双相情感障碍和精神分裂症中起重要作用。然而,关于NOS1AP在神经或精神疾病方面的研究进展尚未得到系统综述。在此,我们介绍NOS1AP的表达、结构和异构体,然后总结NOS1AP的生理作用,并讨论NOS1AP改变与一些神经和精神疾病病理生理学之间的关系。该综述将促进未来对NOS1AP在脑部疾病中的进一步研究以及针对NOS1AP的PTB结构域或PDZ结合基序的药物开发。

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