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Lysine11-Linked Polyubiquitination of the AnkB F-Box Effector of Legionella pneumophila

机译:肺炎军团菌的AnkB F-盒效应子的赖氨酸11连锁的多泛素化。

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摘要

The fate of the polyubiquitinated protein is determined by the lysine linkages involved in the polymerization of the ubiquitin monomers, which has seven lysine residues (K6, K11, K27, K29, K33, K48, and K63). The translocated AnkB effector of the intravacuolar pathogen Legionella pneumophila is a bona fide F-box protein, which is localized to the cytosolic side of the Legionella-containing vacuole (LCV) and is essential for intravacuolar proliferation within macrophages and amoebae. The F-box domain of AnkB interacts with the host SCF1 E3 ubiquitin ligase that triggers the decoration of the LCV with K48-linked polyubiquitinated proteins that are targeted for proteasomal degradation. Here we report that AnkB becomes rapidly polyubiquitinated within the host cell, and this modification is independent of the F-box domain of AnkB, indicating host-mediated polyubiquitination. We show that the AnkB effector interacts specifically with the host E3 ubiquitin ligase Trim21. Mass spectrometry analyses have shown that AnkB is modified by K11-linked polyubiquitination, which has no effect on its stability. This work shows the first example of K11-linked polyubiquitination of a bacterial effector and its interaction with the host Trim21 ubiquitin ligase.
机译:多泛素化蛋白的命运取决于参与泛素单体聚合的赖氨酸键,该赖氨酸键具有七个赖氨酸残基(K 6 ,K 11 ,K 27 ,K 29 ,K 33 ,K 48 和K 63 )。真空内病原体肺炎军团菌的易位AnkB效应子是一种真正的F盒蛋白,其位于含军团菌液泡(LCV)的胞质侧,对于巨噬细胞和变形虫内的真空内增殖至关重要。 AnkB的F-box结构域与宿主SCF1 E3泛素连接酶相互作用,从而触发了以K 48 连接的多泛素化蛋白(针对蛋白酶体降解)修饰LCV。在这里我们报告AnkB在宿主细胞内迅速多聚泛素化,并且此修饰独立于AnkB的F-box域,表明宿主介导的多聚泛素化。我们显示,AnkB效应子与宿主E3泛素连接酶Trim21特异性相互作用。质谱分析表明,AnkB被K 11 连接的多聚泛素修饰,对其稳定性没有影响。这项工作显示了细菌效应子的K 11 连接的多聚泛素化及其与宿主Trim21泛素连接酶的相互作用的第一个例子。

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