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ATP 结合蛋白的富集揭示了白色念珠菌与人巨噬细胞相互作用后细胞死亡、炎症反应和蛋白质合成的蛋白质组学变化。

Enrichment of ATP Binding Proteins Unveils Proteomic Alterations in Human Macrophage Cell Death, Inflammatory Response, and Protein Synthesis after Interaction with Candida albicans.

机构信息

Departamento de Microbiologı́a y Parasitología, Facultad de Farmacia , Universidad Complutense de Madrid , 28040 Madrid , Spain.

Instituto Ramón y Cajal de Investigación Sanitaria IRYCIS , 28034 Madrid , Spain.

出版信息

J Proteome Res. 2019 May 3;18(5):2139-2159. doi: 10.1021/acs.jproteome.9b00032. Epub 2019 Apr 23.

DOI:10.1021/acs.jproteome.9b00032
PMID:30985132
Abstract

Macrophages are involved in the primary human response to Candida albicans. After pathogen recognition, signaling pathways are activated, leading to the production of cytokines, chemokines, and antimicrobial peptides. ATP binding proteins are crucial for this regulation. Here, a quantitative proteomic and phosphoproteomic approach was carried out for the study of human macrophage ATP-binding proteins after interaction with C. albicans. From a total of 547 nonredundant quantified proteins, 137 were ATP binding proteins and 59 were detected as differentially abundant. From the differentially abundant ATP-binding proteins, 6 were kinases (MAP2K2, SYK, STK3, MAP3K2, NDKA, and SRPK1), most of them involved in signaling pathways. Furthermore, 85 phosphopeptides were quantified. Macrophage proteomic alterations including an increase of protein synthesis with a consistent decrease in proteolysis were observed. Besides, macrophages showed changes in proteins of endosomal trafficking together with mitochondrial proteins, including some involved in the response to oxidative stress. Regarding cell death mechanisms, an increase of antiapoptotic over pro-apoptotic signals is suggested. Furthermore, a high pro-inflammatory response was detected, together with no upregulation of key mi-RNAs involved in the negative feedback of this response. These findings illustrate a strategy to deepen the knowledge of the complex interactions between the host and the clinically important pathogen C. albicans.

摘要

巨噬细胞参与了人体对白念珠菌的初始反应。在病原体识别后,信号通路被激活,导致细胞因子、趋化因子和抗菌肽的产生。ATP 结合蛋白在这种调节中至关重要。在这里,我们采用了一种定量蛋白质组学和磷酸化蛋白质组学方法,研究了人类巨噬细胞与白念珠菌相互作用后 ATP 结合蛋白的变化。在总共 547 个非冗余定量蛋白中,有 137 个是 ATP 结合蛋白,有 59 个被检测为差异丰度蛋白。在差异丰度的 ATP 结合蛋白中,有 6 个是激酶(MAP2K2、SYK、STK3、MAP3K2、NDKA 和 SRPK1),其中大多数参与信号通路。此外,还定量了 85 个磷酸肽。观察到巨噬细胞蛋白质组发生了变化,包括蛋白质合成增加,而蛋白酶解一致减少。此外,还观察到内体运输蛋白和线粒体蛋白的变化,包括一些与氧化应激反应有关的蛋白。关于细胞死亡机制,提示抗凋亡信号增加,而促凋亡信号减少。此外,还检测到强烈的促炎反应,而与该反应的负反馈相关的关键 mi-RNAs 没有上调。这些发现说明了一种策略,可以深入了解宿主与临床上重要的病原体白念珠菌之间复杂的相互作用。

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