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基于邻近生物鉴定技术评估 EBV LMP1 的互作组。

The interactome of EBV LMP1 evaluated by proximity-based BioID approach.

机构信息

Department of Biomedical Sciences, Florida State University College of Medicine, Tallahassee, FL 32306, United States.

Department of Biological Sciences, Florida State University, Tallahassee, FL 32306, United States.

出版信息

Virology. 2018 Mar;516:55-70. doi: 10.1016/j.virol.2017.12.033. Epub 2018 Jan 9.

Abstract

Epstein-Barr virus LMP1 is an oncoprotein required for immortalizing B lymphocytes and also plays important roles in transforming non-lymphoid tissue. The discovery of LMP1 protein interactions will likely generate targets to treat EBV-associated cancers. Here, we define the broader LMP1 interactome using the recently developed BioID method. Combined with mass spectrometry, we identified over 1000 proteins across seven independent experiments with direct or indirect relationships to LMP1. Pathway analysis suggests that a significant number of the proteins identified are involved in signal transduction and protein or vesicle trafficking. Interestingly, a large number of proteins thought to be important in the formation of exosomes and protein targeting were recognized as probable LMP1 interacting partners, including CD63, syntenin-1, ALIX, TSG101, HRS, CHMPs, and sorting nexins. Therefore, it is likely that LMP1 modifies protein trafficking and exosome biogenesis pathways. In support of this, knock-down of syntenin-1 and ALIX resulted in reduced exosomal LMP1.

摘要

EB 病毒 LMP1 是一种癌蛋白,它可使 B 淋巴细胞永生化,在转化非淋巴组织方面也发挥重要作用。LMP1 蛋白相互作用的发现可能会产生治疗 EBV 相关癌症的靶点。在这里,我们使用最近开发的 BioID 方法来定义更广泛的 LMP1 相互作用组。通过结合质谱分析,我们在七个独立的实验中鉴定出了 1000 多种与 LMP1 有直接或间接关系的蛋白质。通路分析表明,大量鉴定出的蛋白质参与信号转导和蛋白质或囊泡运输。有趣的是,许多被认为在形成外泌体和蛋白质靶向中非常重要的蛋白质被认为是可能的 LMP1 相互作用伙伴,包括 CD63、syntenin-1、ALIX、TSG101、HRS、CHMPs 和分选连接蛋白。因此,LMP1 很可能修饰蛋白质运输和外泌体生物发生途径。为此,敲低 syntenin-1 和 ALIX 导致外泌体 LMP1 减少。

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