Literature DB >> 19297318

Inhibitory mechanism of Escherichia coli RelE-RelB toxin-antitoxin module involves a helix displacement near an mRNA interferase active site.

Guang-Yao Li1, Yonglong Zhang, Masayori Inouye, Mitsuhiko Ikura.   

Abstract

In Escherichia coli, RelE toxin participates in growth arrest and cell death by inducing mRNA degradation at the ribosomal A-site under stress conditions. The NMR structures of a mutant of E. coli RelE toxin, RelE(R81A/R83A), with reduced toxicity and its complex with an inhibitory peptide from RelB antitoxin, RelB(C) (Lys(47)-Leu(79)), have been determined. In the free RelE(R81A/R83A) structure, helix alpha4 at the C terminus adopts a closed conformation contacting with the beta-sheet core and adjacent loops. In the RelE(R81A/R83A)-RelB(C) complex, helix alpha3(*) of RelB(C) displaces alpha4 of RelE(R81A/R83A) from the binding site on the beta-sheet core. This helix replacement results in neutralization of a conserved positively charged cluster of RelE by acidic residues from alpha3(*) of RelB. The released helix alpha4 becomes unfolded, adopting an open conformation with increased mobility. The displacement of alpha4 disrupts the geometry of critical residues, including Arg(81) and Tyr(87), in a putative active site of RelE toxin. Our structures indicate that RelB counteracts the toxic activity of RelE by displacing alpha4 helix from the catalytically competent position found in the free RelE structure.

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Year:  2009        PMID: 19297318      PMCID: PMC2682910          DOI: 10.1074/jbc.M809656200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  35 in total

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Journal:  Mol Cell       Date:  2005-08-19       Impact factor: 17.970

6.  Structural mechanism of transcriptional autorepression of the Escherichia coli RelB/RelE antitoxin/toxin module.

Authors:  Guang-Yao Li; Yonglong Zhang; Masayori Inouye; Mitsuhiko Ikura
Journal:  J Mol Biol       Date:  2008-04-22       Impact factor: 5.469

7.  The program XEASY for computer-supported NMR spectral analysis of biological macromolecules.

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8.  Protein backbone angle restraints from searching a database for chemical shift and sequence homology.

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10.  Torsion angle dynamics for NMR structure calculation with the new program DYANA.

Authors:  P Güntert; C Mumenthaler; K Wüthrich
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  41 in total

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5.  Structure of the Proteus vulgaris HigB-(HigA)2-HigB toxin-antitoxin complex.

Authors:  Marc A Schureck; Tatsuya Maehigashi; Stacey J Miles; Jhomar Marquez; Shein Ei Cho; Rachel Erdman; Christine M Dunham
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6.  Bacterial toxin RelE mediates frequent codon-independent mRNA cleavage from the 5' end of coding regions in vivo.

Authors:  Jennifer M Hurley; Jonathan W Cruz; Ming Ouyang; Nancy A Woychik
Journal:  J Biol Chem       Date:  2011-02-15       Impact factor: 5.157

7.  A differential effect of E. coli toxin-antitoxin systems on cell death in liquid media and biofilm formation.

Authors:  Ilana Kolodkin-Gal; Reut Verdiger; Ayalla Shlosberg-Fedida; Hanna Engelberg-Kulka
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8.  Three dimensional structure of the MqsR:MqsA complex: a novel TA pair comprised of a toxin homologous to RelE and an antitoxin with unique properties.

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9.  The structural basis for mRNA recognition and cleavage by the ribosome-dependent endonuclease RelE.

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10.  Three new RelE-homologous mRNA interferases of Escherichia coli differentially induced by environmental stresses.

Authors:  Mikkel Christensen-Dalsgaard; Mikkel Girke Jørgensen; Kenn Gerdes
Journal:  Mol Microbiol       Date:  2009-11-25       Impact factor: 3.501

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