Boyle Keith B, Thurston Teresa L M, Randow Felix
a MRC Laboratory of Molecular Biology, Division of Protein and Nucleic Acid Chemistry, Francis Crick Avenue , Cambridge , UK.
b MRC Center for Molecular Bacteriology and Infection , Imperial College, London, Flowers Building, Exhibition Road, London , UK.
Autophagy. 2016 Dec;12(12):2508-2509. doi: 10.1080/15548627.2016.1235126. Epub 2016 Oct 18.
Defense of the mammalian cell cytosol against Salmonella invasion is reliant upon capture of the infiltrating bacteria by macroautophagy (hereafter autophagy), a process controlled by the kinase TBK1. In our recent study we showed that recruitment of TBK1 activity to Salmonella stabilizes the key autophagy regulator WIPI2 on those bacteria, a novel and essential function for TBK1 in the control of the early steps of antibacterial autophagy. Substantial redundancy exists in the precise recruitment mechanism for TBK1 because engagement with any of several Salmonella-associated 'eat-me' signals, including host-derived glycans, and K48- and K63-linked ubiquitin chains, suffices to recruit TBK1 functionality. We therefore propose that buffering TBK1 recruitment against potential bacterial interference might be of evolutionary advantage to the host.
哺乳动物细胞胞质溶胶抵御沙门氏菌入侵依赖于通过巨自噬(以下简称自噬)捕获浸润细菌,这一过程由激酶TBK1控制。在我们最近的研究中,我们表明将TBK1活性募集到沙门氏菌上可使关键自噬调节因子WIPI2在这些细菌上稳定,这是TBK1在控制抗菌自噬早期步骤中的一种新的重要功能。TBK1的精确募集机制存在大量冗余,因为与几种沙门氏菌相关的“吃我”信号中的任何一种结合,包括宿主来源的聚糖以及K48和K63连接的泛素链,都足以募集TBK1功能。因此,我们提出缓冲TBK1募集以对抗潜在的细菌干扰可能对宿主具有进化优势。
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