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      Threonine eliminylation by bacterial phosphothreonine lyases rapidly causes cross-linking of mitogen-activated protein kinase (MAPK) in live cells

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          Abstract

          Old long-lived proteins contain dehydroalanine (Dha) and dehydrobutyrine (Dhb), two amino acids engendered by dehydration of serines and threonines, respectively. Although these residues have a suspected role in protein cross-linking and aggregation, their direct implication has yet to be determined. Here, we have taken advantage of the ability of the enteropathogen Shigella to convert the phosphothreonine residue of the pT- X-pY consensus sequence of ERK and p38 into Dhb and followed the impact of dehydration on the fate of the two MAPKs. To that end, we have generated the first antibodies recognizing Dhb-modified proteins and allowing tracing them as they form. We showed that Dhb modifications accumulate in a long-lasting manner in Shigella-infected cells, causing subsequent formation of covalent cross-links of MAPKs. Moreover, the Dhb signal correlates precisely with the activation of the Shigella type III secretion apparatus, thus evidencing injectisome activity. This observation is the first to document a causal link between Dhb formation and protein cross-linking in live cells. Detection of eliminylation is a new avenue to phosphoproteome regulation in eukaryotes that will be instrumental for the development of type III secretion inhibitors.

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          Author and article information

          Journal
          J Biol Chem
          J. Biol. Chem
          jbc
          jbc
          JBC
          The Journal of Biological Chemistry
          American Society for Biochemistry and Molecular Biology (11200 Rockville Pike, Suite 302, Rockville, MD 20852-3110, U.S.A. )
          0021-9258
          1083-351X
          12 May 2017
          21 March 2017
          : 292
          : 19
          : 7784-7794
          Affiliations
          From the []Team genomic plasticity and infection, Department of Immunology, Infectiology and Hematology, Institut Necker Enfants Malades, INSERM U1151, CNRS UMR 8253, 75993 Paris CEDEX 14, France,
          [‖‖ ]Université Paris Descartes,75270 Paris CEDEX 06, France,
          the [§ ]Université Paris Diderot, Sorbonne Paris Cité, Cellule Pasteur UPMC, 75724 Paris, France,
          []Institut Pasteur, Department of Biologie du Développement et Cellules Souches, Unité de Régulation Epigénétique, 75724 Paris CEDEX 15, France
          []UMR3738 CNRS, 75732 Paris CEDEX 15, France,
          the [** ]Proteomic Platform Necker, PPN-3P5, Structure Fédérative de Recherche SFR Necker US24, 75015 Paris, France,
          the [‡‡ ]CPN Proteomics Facility–3P5, Center of Psychiatry and Neuroscience, UMR INSERM 894, 75014 Paris, France,
          the [§§ ]Unité de Chimie des Biomolécules, Institut Pasteur, 75015 Paris, France, and
          the [¶¶ ]Unité de Pathogénie Microbienne Moléculaire, Unité INSERM U1202, Institut Pasteur, 75015 Paris, France
          Author notes
          [2 ] To whom correspondence should be addressed. E-mail: laurence.arbibe@ 123456inserm.fr .
          [1]

          Present address: School of Life Sciences, EPFL, Lausanne, Switzerland.

          Edited by Gerald W. Hart

          Article
          PMC5427260 PMC5427260 5427260 M117.775940
          10.1074/jbc.M117.775940
          5427260
          28325837
          4adda908-248c-443d-b182-ad06c866ab20
          © 2017 by The American Society for Biochemistry and Molecular Biology, Inc.
          History
          : 9 January 2016
          : 21 March 2017
          Categories
          Genomics and Proteomics

          aging,bacterial protein phosphatase,mitogen-activated protein kinase (MAPK),phosphoproteomics,protein aggregation,type III secretion system (T3SS),Shigella,dehydroalanine,dehydrobutyrine,protein cross-link

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