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次氯酸诱导修饰对磷酸酶和张力蛋白同源物(PTEN)结构和功能的影响。

The effect of HOCl-induced modifications on phosphatase and tensin homologue (PTEN) structure and function.

机构信息

a School of Life and Health Sciences , Aston University , Birmingham , UK.

出版信息

Free Radic Res. 2018 Feb;52(2):232-247. doi: 10.1080/10715762.2018.1424333. Epub 2018 Jan 22.

DOI:10.1080/10715762.2018.1424333
PMID:29298524
Abstract

Oxidation by reactive species can cause changes in protein function and affect cell signalling pathways. Phosphatase and tensin homologue (PTEN) is a negative regulator of the PI3K/AKT pathway and is known to be inhibited by oxidation, but its oxidation by the myeloperoxidase-derived oxidant hypochlorous acid (HOCl) has not previously been investigated. PTEN-GST was treated with HOCl:protein ratios from 15:1 to 300:1. Decreases in PTEN phosphatase activity were observed at treatment ratios of 60:1 and higher, which correlated with the loss of the intact protein band and appearance of high molecular weight aggregates in SDS-PAGE. LC-MSMS was used to map oxidative modifications (oxPTMs) in PTEN-GST tryptic peptides and label-free quantitative proteomics used to determine their relative abundance. Twenty different oxPTMs of PTEN were identified, of which 14 were significantly elevated upon HOCl treatment in a dose-dependent manner. Methionine and cysteine residues were the most heavily oxidised; the percentage modification depended on their location in the sequence, reflecting differences in susceptibility. Other modifications included tyrosine chlorination and dichlorination, and hydroxylations of tyrosine, tryptophan, and proline. Much higher levels of oxidation occurred in the protein aggregates compared to the monomeric protein for certain methionine and tyrosine residues located in the C2 and C-terminal domains, suggesting that their oxidation promoted protein destabilisation and aggregation; many of the residues modified were classified as buried according to their solvent accessibility. This study provides novel information on the susceptibility of PTEN to the inflammatory oxidant HOCl and its effects on the structure and activity of the protein.

摘要

活性氧物质的氧化作用会导致蛋白质功能发生变化,并影响细胞信号通路。磷酸酶和张力蛋白同源物(PTEN)是 PI3K/AKT 通路的负调节剂,已知其氧化作用会受到抑制,但此前尚未研究过髓过氧化物酶衍生的氧化剂次氯酸(HOCl)对其的氧化作用。将 PTEN-GST 与 HOCl: 蛋白比从 15:1 至 300:1 进行处理。在处理比为 60:1 及更高时,观察到 PTEN 磷酸酶活性降低,这与完整蛋白质带的丢失以及 SDS-PAGE 中出现高分子量聚集体相关。LC-MSMS 用于对 PTEN-GST 胰蛋白酶肽中的氧化修饰(oxPTMs)进行作图,并用无标记定量蛋白质组学来确定它们的相对丰度。鉴定出了 20 种不同的 PTEN oxPTMs,其中 14 种在 HOCl 处理时呈剂量依赖性显著升高。蛋氨酸和半胱氨酸残基的氧化程度最高;修饰百分比取决于其在序列中的位置,反映了易感性的差异。其他修饰包括酪氨酸的氯化和二氯化,以及酪氨酸、色氨酸和脯氨酸的羟基化。与单体蛋白相比,某些位于 C2 和 C 末端结构域中的蛋氨酸和酪氨酸残基在蛋白质聚集体中发生了更高水平的氧化,这表明其氧化作用促进了蛋白质的不稳定性和聚集;许多被修饰的残基根据其溶剂可及性被归类为埋藏残基。本研究提供了有关 PTEN 对炎症性氧化剂 HOCl 的易感性及其对蛋白质结构和活性的影响的新信息。

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