Insights into the Mechanism of Type I Dehydroquinate Dehydratases from Structures of Reaction Intermediates

Light, Samuel H; Minasov, George; Shuvalova, Ludmilla; Duban, Mark-Eugene; Caffrey, Michael; Anderson, Wayne F; Lavie, Arnon

doi:10.1074/jbc.M110.192831

Insights into the Mechanism of Type I Dehydroquinate Dehydratases from Structures of Reaction Intermediates

Journal Article · Sun Feb 26 23:00:00 EST 2012 · J. Biol. Chem.

DOI:https://doi.org/10.1074/jbc.M110.192831· OSTI ID:1034207

Light, Samuel H; Minasov, George; Shuvalova, Ludmilla; Duban, Mark-Eugene; Caffrey, Michael; Anderson, Wayne F; Lavie, Arnon ^[1]

NWU

The biosynthetic shikimate pathway consists of seven enzymes that catalyze sequential reactions to generate chorismate, a critical branch point in the synthesis of the aromatic amino acids. The third enzyme in the pathway, dehydroquinate dehydratase (DHQD), catalyzes the dehydration of 3-dehydroquinate to 3-dehydroshikimate. We present three crystal structures of the type I DHQD from the intestinal pathogens Clostridium difficile and Salmonella enterica. Structures of the enzyme with substrate and covalent pre- and post-dehydration reaction intermediates provide snapshots of successive steps along the type I DHQD-catalyzed reaction coordinate. These structures reveal that the position of the substrate within the active site does not appreciably change upon Schiff base formation. The intermediate state structures reveal a reaction state-dependent behavior of His-143 in which the residue adopts a conformation proximal to the site of catalytic dehydration only when the leaving group is present. We speculate that His-143 is likely to assume differing catalytic roles in each of its observed conformations. One conformation of His-143 positions the residue for the formation/hydrolysis of the covalent Schiff base intermediates, whereas the other conformation positions the residue for a role in the catalytic dehydration event. The fact that the shikimate pathway is absent from humans makes the enzymes of the pathway potential targets for the development of non-toxic antimicrobials. The structures and mechanistic insight presented here may inform the design of type I DHQD enzyme inhibitors.

Research Organization:: Advanced Photon Source (APS), Argonne National Laboratory (ANL), Argonne, IL (US)

Sponsoring Organization:: NIH

OSTI ID:: 1034207

Journal Information:: J. Biol. Chem., Journal Name: J. Biol. Chem. Journal Issue: (5) ; 02, 2011 Vol. 286; ISSN JBCHA3; ISSN 0021-9258

Country of Publication:: United States

Language:: ENGLISH

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Related Subjects

59 BASIC BIOLOGICAL SCIENCES
60 APPLIED LIFE SCIENCES
AMINO ACIDS
ANTIBIOTICS
AROMATICS
CATALYSIS
CLOSTRIDIUM
CRYSTAL STRUCTURE
CRYSTALLOGRAPHY
DEHYDRATION
DESIGN
ENZYME INHIBITORS
ENZYMES
METABOLISM
PATHOGENS
REACTION INTERMEDIATES
RESIDUES
SALMONELLA
SCHIFF BASES
SUBSTRATES
SYNTHESIS
TARGETS

Insights into the Mechanism of Type I Dehydroquinate Dehydratases from Structures of Reaction Intermediates

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