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棘手的情况:蛋白质棕榈酰化的调节与功能,聚焦于轴突和轴突起始段

A sticky situation: regulation and function of protein palmitoylation with a spotlight on the axon and axon initial segment.

作者信息

Petropavlovskiy Andrey A, Kogut Jordan A, Leekha Arshia, Townsend Charlotte A, Sanders Shaun S

机构信息

Department of Molecular and Cellular Biology, University of Guelph, 50 Stone Rd E, Guelph N1G 2W1, Ontario, Canada.

出版信息

Neuronal Signal. 2021 Oct 6;5(4):NS20210005. doi: 10.1042/NS20210005. eCollection 2021 Dec.

Abstract

In neurons, the axon and axon initial segment (AIS) are critical structures for action potential initiation and propagation. Their formation and function rely on tight compartmentalisation, a process where specific proteins are trafficked to and retained at distinct subcellular locations. One mechanism which regulates protein trafficking and association with lipid membranes is the modification of protein cysteine residues with the 16-carbon palmitic acid, known as S-acylation or palmitoylation. Palmitoylation, akin to phosphorylation, is reversible, with palmitate cycling being mediated by substrate-specific enzymes. Palmitoylation is well-known to be highly prevalent among neuronal proteins and is well studied in the context of the synapse. Comparatively, how palmitoylation regulates trafficking and clustering of axonal and AIS proteins remains less understood. This review provides an overview of the current understanding of the biochemical regulation of palmitoylation, its involvement in various neurological diseases, and the most up-to-date perspective on axonal palmitoylation. Through a palmitoylation analysis of the AIS proteome, we also report that an overwhelming proportion of AIS proteins are likely palmitoylated. Overall, our review and analysis confirm a central role for palmitoylation in the formation and function of the axon and AIS and provide a resource for further exploration of palmitoylation-dependent protein targeting to and function at the AIS.

摘要

在神经元中,轴突和轴突起始段(AIS)是动作电位起始和传播的关键结构。它们的形成和功能依赖于紧密的区室化,即特定蛋白质被运输到不同的亚细胞位置并保留在那里的过程。一种调节蛋白质运输以及与脂质膜结合的机制是用16碳的棕榈酸修饰蛋白质半胱氨酸残基,这一过程称为S-酰化或棕榈酰化。与磷酸化类似,棕榈酰化是可逆的,棕榈酸循环由底物特异性酶介导。众所周知,棕榈酰化在神经元蛋白质中非常普遍,并且在突触的背景下已得到充分研究。相比之下,棕榈酰化如何调节轴突和AIS蛋白质的运输和聚集仍不太清楚。本综述概述了目前对棕榈酰化生化调节的理解、其在各种神经疾病中的作用,以及关于轴突棕榈酰化的最新观点。通过对AIS蛋白质组的棕榈酰化分析,我们还报告称,绝大多数AIS蛋白质可能被棕榈酰化。总体而言,我们的综述和分析证实了棕榈酰化在轴突和AIS形成及功能中的核心作用,并为进一步探索依赖棕榈酰化的蛋白质靶向AIS及在AIS发挥功能提供了资源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9bef/8495546/b37a20f70fe2/ns-05-ns20210005C-g1.jpg

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