Structure of a novel antibacterial toxin that exploits elongation factor Tu to cleave specific transfer RNAs

Contact-dependent growth inhibition (CDI) is a mechanism of inter-cellular competition in which Gram-negative bacteria exchange polymorphic toxins using type V secretion systems. Here, we present structures of the CDI toxin from Escherichia coli NC101 in ternary complex with its cognate immunity pro...

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Autores principales: Michalska, Karolina, Gucinski, Grant C., Garza-Sánchez, Fernando, Johnson, Parker M., Stols, Lucy M., Eschenfeldt, William H., Babnigg, Gyorgy, Low, David A., Goulding, Celia W., Joachimiak, Andrzej, Hayes, Christopher S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2017
Materias:
Structural Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5737660/
https://www.ncbi.nlm.nih.gov/pubmed/28973472
http://dx.doi.org/10.1093/nar/gkx700
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author Michalska, Karolina
Gucinski, Grant C.
Garza-Sánchez, Fernando
Johnson, Parker M.
Stols, Lucy M.
Eschenfeldt, William H.
Babnigg, Gyorgy
Low, David A.
Goulding, Celia W.
Joachimiak, Andrzej
Hayes, Christopher S.
author_facet Michalska, Karolina
Gucinski, Grant C.
Garza-Sánchez, Fernando
Johnson, Parker M.
Stols, Lucy M.
Eschenfeldt, William H.
Babnigg, Gyorgy
Low, David A.
Goulding, Celia W.
Joachimiak, Andrzej
Hayes, Christopher S.
author_sort Michalska, Karolina
collection PubMed
description Contact-dependent growth inhibition (CDI) is a mechanism of inter-cellular competition in which Gram-negative bacteria exchange polymorphic toxins using type V secretion systems. Here, we present structures of the CDI toxin from Escherichia coli NC101 in ternary complex with its cognate immunity protein and elongation factor Tu (EF-Tu). The toxin binds exclusively to domain 2 of EF-Tu, partially overlapping the site that interacts with the 3′-end of aminoacyl-tRNA (aa-tRNA). The toxin exerts a unique ribonuclease activity that cleaves the single-stranded 3′-end from tRNAs that contain guanine discriminator nucleotides. EF-Tu is required to support this tRNase activity in vitro, suggesting the toxin specifically cleaves substrate in the context of GTP·EF-Tu·aa-tRNA complexes. However, superimposition of the toxin domain onto previously solved GTP·EF-Tu·aa-tRNA structures reveals potential steric clashes with both aa-tRNA and the switch I region of EF-Tu. Further, the toxin induces conformational changes in EF-Tu, displacing a β-hairpin loop that forms a critical salt-bridge contact with the 3′-terminal adenylate of aa-tRNA. Together, these observations suggest that the toxin remodels GTP·EF-Tu·aa-tRNA complexes to free the 3′-end of aa-tRNA for entry into the nuclease active site.
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spelling pubmed-57376602018-01-04 Structure of a novel antibacterial toxin that exploits elongation factor Tu to cleave specific transfer RNAs Michalska, Karolina Gucinski, Grant C. Garza-Sánchez, Fernando Johnson, Parker M. Stols, Lucy M. Eschenfeldt, William H. Babnigg, Gyorgy Low, David A. Goulding, Celia W. Joachimiak, Andrzej Hayes, Christopher S. Nucleic Acids Res Structural Biology Contact-dependent growth inhibition (CDI) is a mechanism of inter-cellular competition in which Gram-negative bacteria exchange polymorphic toxins using type V secretion systems. Here, we present structures of the CDI toxin from Escherichia coli NC101 in ternary complex with its cognate immunity protein and elongation factor Tu (EF-Tu). The toxin binds exclusively to domain 2 of EF-Tu, partially overlapping the site that interacts with the 3′-end of aminoacyl-tRNA (aa-tRNA). The toxin exerts a unique ribonuclease activity that cleaves the single-stranded 3′-end from tRNAs that contain guanine discriminator nucleotides. EF-Tu is required to support this tRNase activity in vitro, suggesting the toxin specifically cleaves substrate in the context of GTP·EF-Tu·aa-tRNA complexes. However, superimposition of the toxin domain onto previously solved GTP·EF-Tu·aa-tRNA structures reveals potential steric clashes with both aa-tRNA and the switch I region of EF-Tu. Further, the toxin induces conformational changes in EF-Tu, displacing a β-hairpin loop that forms a critical salt-bridge contact with the 3′-terminal adenylate of aa-tRNA. Together, these observations suggest that the toxin remodels GTP·EF-Tu·aa-tRNA complexes to free the 3′-end of aa-tRNA for entry into the nuclease active site. Oxford University Press 2017-09-29 2017-08-11 /pmc/articles/PMC5737660/ /pubmed/28973472 http://dx.doi.org/10.1093/nar/gkx700 Text en © The Author(s) 2017. Published by Oxford University Press on behalf of Nucleic Acids Research. http://creativecommons.org/licenses/by-nc/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Structural Biology
Michalska, Karolina
Gucinski, Grant C.
Garza-Sánchez, Fernando
Johnson, Parker M.
Stols, Lucy M.
Eschenfeldt, William H.
Babnigg, Gyorgy
Low, David A.
Goulding, Celia W.
Joachimiak, Andrzej
Hayes, Christopher S.
Structure of a novel antibacterial toxin that exploits elongation factor Tu to cleave specific transfer RNAs
title Structure of a novel antibacterial toxin that exploits elongation factor Tu to cleave specific transfer RNAs
title_full Structure of a novel antibacterial toxin that exploits elongation factor Tu to cleave specific transfer RNAs
title_fullStr Structure of a novel antibacterial toxin that exploits elongation factor Tu to cleave specific transfer RNAs
title_full_unstemmed Structure of a novel antibacterial toxin that exploits elongation factor Tu to cleave specific transfer RNAs
title_short Structure of a novel antibacterial toxin that exploits elongation factor Tu to cleave specific transfer RNAs
title_sort structure of a novel antibacterial toxin that exploits elongation factor tu to cleave specific transfer rnas
topic Structural Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5737660/
https://www.ncbi.nlm.nih.gov/pubmed/28973472
http://dx.doi.org/10.1093/nar/gkx700
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