Literature DB >> 19692332

Structural basis for substrate recognition in the enzymatic component of ADP-ribosyltransferase toxin CDTa from Clostridium difficile.

Amit Sundriyal1, April K Roberts, Clifford C Shone, K Ravi Acharya.   

Abstract

ADP-ribosylation is one of the favored modes of cell intoxication employed by several bacteria. Clostridium difficile is recognized to be an important nosocomial pathogen associated with considerable morbidity and attributable mortality. Along with its two well known toxins, Toxin A and Toxin B, it produces an ADP-ribosylating toxin that targets monomeric actin of the target cell. Like other Clostridial actin ADP-ribosylating toxins, this binary toxin, known as C. difficile toxin (CDT), is composed of two subunits, CDTa and CDTb. In this study, we present high resolution crystal structures of CDTa in its native form (at pH 4.0, 8.5, and 9.0) and in complex with ADP-ribose donors, NAD and NADPH (at pH 9.0). The crystal structures of the native protein show "pronounced conformational flexibility" confined to the active site region of the protein and "enhanced" disorder at low pH, whereas the complex structures highlight significant differences in "ligand specificity" compared with the enzymatic subunit of a close homologue, Clostridium perfringens iota toxin. Specifically in CDTa, two of the suggested catalytically important residues (Glu-385 and Glu-387) seem to play no role or a less important role in ligand binding. These structural data provide the first detailed information on protein-donor substrate complex stabilization in CDTa, which may have implications in understanding CDT recognition.

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Year:  2009        PMID: 19692332      PMCID: PMC2781416          DOI: 10.1074/jbc.M109.043018

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


  30 in total

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2.  Refinement of macromolecular structures by the maximum-likelihood method.

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Authors:  Daniel E Voth; Jimmy D Ballard
Journal:  Clin Microbiol Rev       Date:  2005-04       Impact factor: 26.132

Review 6.  A family of killer toxins. Exploring the mechanism of ADP-ribosylating toxins.

Authors:  Kenneth P Holbourn; Clifford C Shone; K R Acharya
Journal:  FEBS J       Date:  2006-09-05       Impact factor: 5.542

7.  Evolution and mechanism from structures of an ADP-ribosylating toxin and NAD complex.

Authors:  S Han; J A Craig; C D Putnam; N B Carozzi; J A Tainer
Journal:  Nat Struct Biol       Date:  1999-10

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Authors:  Holger Barth; Klaus Aktories; Michel R Popoff; Bradley G Stiles
Journal:  Microbiol Mol Biol Rev       Date:  2004-09       Impact factor: 11.056

10.  Crystal structure and site-directed mutagenesis of enzymatic components from Clostridium perfringens iota-toxin.

Authors:  Hideaki Tsuge; Masahiro Nagahama; Hiroyuki Nishimura; Junzo Hisatsune; Yoshihiko Sakaguchi; Yasuhiro Itogawa; Nobuhiko Katunuma; Jun Sakurai
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  25 in total

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Journal:  J Biol Chem       Date:  2012-04-25       Impact factor: 5.157

2.  Rho GTPase Recognition by C3 Exoenzyme Based on C3-RhoA Complex Structure.

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Review 3.  Obstructing toxin pathways by targeted pore blockage.

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4.  Arginine ADP-ribosylation mechanism based on structural snapshots of iota-toxin and actin complex.

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Review 5.  Clostridium difficile infection.

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Review 6.  The role of toxins in Clostridium difficile infection.

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7.  Structural elucidation of the Clostridioides difficile transferase toxin reveals a single-site binding mode for the enzyme.

Authors:  Michael J Sheedlo; David M Anderson; Audrey K Thomas; D Borden Lacy
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Review 8.  Clostridium difficile toxins: mediators of inflammation.

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Journal:  J Innate Immun       Date:  2012-01-10       Impact factor: 7.349

9.  1H, 13C, and 15N resonance assignments of an enzymatically active domain from the catalytic component (CDTa, residues 216-420) of a binary toxin from Clostridium difficile.

Authors:  Braden M Roth; Raquel Godoy-Ruiz; Kristen M Varney; Richard R Rustandi; David J Weber
Journal:  Biomol NMR Assign       Date:  2016-02-17       Impact factor: 0.746

Review 10.  Structural biology of the writers, readers, and erasers in mono- and poly(ADP-ribose) mediated signaling.

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