Substrate recognition and cryo-EM structure of the ribosome-bound TAC toxin of Mycobacterium tuberculosis

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作者
Moise Mansour
Emmanuel Giudice
Xibing Xu
Hatice Akarsu
Patricia Bordes
Valérie Guillet
Donna-Joe Bigot
Nawel Slama
Gaetano D’urso
Sophie Chat
Peter Redder
Laurent Falquet
Lionel Mourey
Reynald Gillet
Pierre Genevaux
机构
[1] Université de Toulouse,Laboratoire de Microbiologie et de Génétique Moléculaires, Centre de Biologie Intégrative (CBI)
[2] CNRS,Department of Biology
[3] UPS,Institut de Pharmacologie et de Biologie Structurale, IPBS
[4] Institut de Génétique et Développement de Rennes (IGDR),Institute of Veterinary Bacteriology
[5] UMR6290,undefined
[6] Université de Rennes,undefined
[7] CNRS,undefined
[8] University of Fribourg & Swiss Institute of Bioinformatics,undefined
[9] Université de Toulouse,undefined
[10] CNRS,undefined
[11] UPS,undefined
[12] University of Bern,undefined
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摘要
Toxins of toxin-antitoxin systems use diverse mechanisms to control bacterial growth. Here, we focus on the deleterious toxin of the atypical tripartite toxin-antitoxin-chaperone (TAC) system of Mycobacterium tuberculosis, whose inhibition requires the concerted action of the antitoxin and its dedicated SecB-like chaperone. We show that the TAC toxin is a bona fide ribonuclease and identify exact cleavage sites in mRNA targets on a transcriptome-wide scale in vivo. mRNA cleavage by the toxin occurs after the second nucleotide of the ribosomal A-site codon during translation, with a strong preference for CCA codons in vivo. Finally, we report the cryo-EM structure of the ribosome-bound TAC toxin in the presence of native M. tuberculosis cspA mRNA, revealing the specific mechanism by which the TAC toxin interacts with the ribosome and the tRNA in the P-site to cleave its mRNA target.
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