Molecular mechanism of toxin neutralization in the HipBST toxin-antitoxin system of Legionella pneumophila

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作者
Xiangkai Zhen
Yongyu Wu
Jinli Ge
Jiaqi Fu
Le Ye
Niannian Lin
Zhijie Huang
Zihe Liu
Zhao-qing Luo
Jiazhang Qiu
Songying Ouyang
机构
[1] Fujian Normal University,Provincial University Key Laboratory of Cellular Stress Response and Metabolic Regulation, the Key Laboratory of Innate Immune Biology of Fujian Province, Biomedical Research Center of South China, Key Laboratory of OptoElectronic
[2] Jilin University,State Key Laboratory for Zoonotic Diseases, College of Veterinary Medicine
[3] Purdue University,Purdue Institute for Inflammation, Immunology and Infectious Disease and Department of Biological Sciences
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Nature Communications | / 13卷
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摘要
Toxin-antitoxin (TA) systems are ubiquitous genetic modules in bacteria and archaea. Here, we perform structural and biochemical characterization of the Legionella pneumophila effector Lpg2370, demonstrating that it is a Ser/Thr kinase. Together with two upstream genes, lpg2370 constitutes the tripartite HipBST TA. Notably, the toxin Lpg2370 (HipTLp) and the antitoxin Lpg2369 (HipSLp) correspond to the C-terminus and N-terminus of HipA from HipBA TA, respectively. By determining crystal structures of autophosphorylated HipTLp, its complex with AMP-PNP, and the structure of HipTLp-HipSLp complex, we identify residues in HipTLp critical for ATP binding and those contributing to its interactions with HipSLp. Structural analysis reveals that HipSLp binding induces a loop-to-helix shift in the P-loop of HipTLp, leading to the blockage of ATP binding and inhibition of the kinase activity. These findings establish the L. pneumophila effector Lpg2370 as the HipBST TA toxin and elucidate the molecular basis for HipT neutralization in HipBST TA.
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