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Insights Into Protein S-Palmitoylation in Synaptic Plasticity and Neurological Disorders: Potential and Limitations of Methods for Detection and Analysis

机译:深入了解突触可塑性和神经系统疾病中的蛋白S-棕榈酸酯化:检测和分析方法的潜力和局限性

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摘要

S-palmitoylation (S-PALM) is a lipid modification that involves the linkage of a fatty acid chain to cysteine residues of the substrate protein. This common posttranslational modification (PTM) is unique among other lipid modifications because of its reversibility. Hence, like phosphorylation or ubiquitination, it can act as a switch that modulates various important physiological pathways within the cell. Numerous studies revealed that S-PALM plays a crucial role in protein trafficking and function throughout the nervous system. Notably, the dynamic turnover of palmitate on proteins at the synapse may provide a key mechanism for rapidly changing synaptic strength. Indeed, palmitate cycling on postsynaptic density-95 (PSD-95), the major postsynaptic density protein at excitatory synapses, regulates the number of synaptic α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptors (AMPARs) and thus affects synaptic transmission. Accumulating evidence suggests a relationship between impairments in S-PALM and severe neurological disorders. Therefore, determining the precise levels of S-PALM may be essential for understanding the ways in which this PTM is regulated in the brain and controls synaptic dynamics. Protein S-PALM can be characterized using metabolic labeling methods and biochemical tools. Both approaches are discussed herein in the context of specific methods and their advantages and disadvantages. This review clearly shows progress in the field, which has led to the development of new, more sensitive techniques that enable the detection of palmitoylated proteins and allow predictions of potential palmitate binding sites. Unfortunately, one significant limitation of these approaches continues to be the inability to use them in living cells.
机译:S-棕榈酰化(S-PALM)是一种脂质修饰,涉及脂肪酸链与底物蛋白的半胱氨酸残基的连接。由于其可逆性,这种常见的翻译后修饰(PTM)在其他脂质修饰中是独一无二的。因此,就像磷酸化或泛素化一样,它可以充当调节细胞内各种重要生理途径的开关。大量研究表明,S-PALM在整个神经系统的蛋白质运输和功能中起着至关重要的作用。值得注意的是,在突触上蛋白质上的棕榈酸酯的动态转换可能提供快速改变突触强度的关键机制。确实,棕榈酸酯在突触后密度95(PSD-95)(兴奋性突触中的主要突触后密度蛋白)上循环,可调节突触α-氨基-3-羟基-5-羟基-5-甲基-4-异恶唑丙酸受体(AMPAR)的数量和因此影响突触传递。越来越多的证据表明,S-PALM损伤与严重的神经系统疾病之间存在关联。因此,确定S-PALM的精确水平对于理解PTM在大脑中的调节方式和控制突触动力学的方式可能至关重要。可以使用代谢标记方法和生化工具来表征蛋白S-PALM。本文在特定方法及其优点和缺点的上下文中讨论了这两种方法。这篇综述清楚地表明了该领域的进展,从而导致了新的,更灵敏的技术的发展,这些技术能够检测棕榈酰化的蛋白质并预测潜在的棕榈酸酯结合位点。不幸的是,这些方法的一个重大局限性仍然是无法在活细胞中使用它们。

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