Structural basis for the toxicity of Legionella pneumophila effector SidH

Author:

Sharma RahulORCID,Adams Michael,Griffith-Jones SimonneORCID,Sahr Tobias,Gomez-Valero Laura,Weis FelixORCID,Hons MichaelORCID,Gharbi SarahORCID,Berkane RayeneORCID,Stolz AlexandraORCID,Buchrieser CarmenORCID,Bhogaraju SagarORCID

Abstract

AbstractLegionella pneumophila (LP) secretes more than 300 effectors into the host cytosol to facilitate intracellular replication. One of these effectors, SidH, 253 kDa in size with no sequence similarity to proteins of known function is toxic when overexpressed in host cells. SidH is regulated by the LP metaeffector LubX which targets SidH for degradation in a temporal manner during LP infection. The mechanism underlying the toxicity of SidH and its role in LP infection are unknown. Here, we determined the cryo-EM structure of SidH at 2.7 Å revealing a unique alpha helical arrangement with no overall similarity to known protein structures. Surprisingly, purified SidH came bound to a E. coli EF-Tu/t-RNA/GTP ternary complex which could be modeled into the cryo-EM density. Mutation of residues disrupting the SidH-tRNA interface and SidH-EF-Tu interface abolish the toxicity of overexpressed SidH in human cells, a phenotype confirmed in infection of Acanthamoeba castellani. We also present the cryo-EM structure of SidH in complex with a U-box domain containing ubiquitin ligase LubX delineating the mechanism of regulation of SidH. Our data provide the basis for the toxicity of SidH and into its regulation by the metaeffector LubX.

Funder

Université Grenoble Alpes

Agence Nationale de la Recherche

Fondation pour la Recherche Médicale

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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