Literature DB >> 18585390

The molecular structure of epoxide hydrolase B from Mycobacterium tuberculosis and its complex with a urea-based inhibitor.

Bichitra K Biswal1, Christophe Morisseau, Grace Garen, Maia M Cherney, Craig Garen, Chunying Niu, Bruce D Hammock, Michael N G James.   

Abstract

Mycobacterium tuberculosis (Mtb), the intracellular pathogen that infects macrophages primarily, is the causative agent of the infectious disease tuberculosis in humans. The Mtb genome encodes at least six epoxide hydrolases (EHs A to F). EHs convert epoxides to trans-dihydrodiols and have roles in drug metabolism as well as in the processing of signaling molecules. Herein, we report the crystal structures of unbound Mtb EHB and Mtb EHB bound to a potent, low-nanomolar (IC(50) approximately 19 nM) urea-based inhibitor at 2.1 and 2.4 A resolution, respectively. The enzyme is a homodimer; each monomer adopts the classical alpha/beta hydrolase fold that composes the catalytic domain; there is a cap domain that regulates access to the active site. The catalytic triad, comprising Asp104, His333 and Asp302, protrudes from the catalytic domain into the substrate binding cavity between the two domains. The urea portion of the inhibitor is bound in the catalytic cavity, mimicking, in part, the substrate binding; the two urea nitrogen atoms donate hydrogen bonds to the nucleophilic carboxylate of Asp104, and the carbonyl oxygen of the urea moiety receives hydrogen bonds from the phenolic oxygen atoms of Tyr164 and Tyr272. The phenolic oxygen groups of these two residues provide electrophilic assistance during the epoxide hydrolytic cleavage. Upon inhibitor binding, the binding-site residues undergo subtle structural rearrangement. In particular, the side chain of Ile137 exhibits a rotation of around 120 degrees about its C(alpha)-C(beta) bond in order to accommodate the inhibitor. These findings have not only shed light on the enzyme mechanism but also have opened a path for the development of potent inhibitors with good pharmacokinetic profiles against all Mtb EHs of the alpha/beta type.

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Year:  2008        PMID: 18585390      PMCID: PMC2866126          DOI: 10.1016/j.jmb.2008.06.030

Source DB:  PubMed          Journal:  J Mol Biol        ISSN: 0022-2836            Impact factor:   5.469


  30 in total

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2.  ESPript/ENDscript: Extracting and rendering sequence and 3D information from atomic structures of proteins.

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3.  Characterization of mycobacterial virulence genes through genetic interaction mapping.

Authors:  Swati M Joshi; Amit K Pandey; Nicole Capite; Sarah M Fortune; Eric J Rubin; Christopher M Sassetti
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4.  Cloning, expression, purification, crystallization and preliminary X-ray studies of epoxide hydrolases A and B from Mycobacterium tuberculosis.

Authors:  Bichitra K Biswal; Grace Garen; Maia M Cherney; Craig Garen; Michael N G James
Journal:  Acta Crystallogr Sect F Struct Biol Cryst Commun       Date:  2006-01-27

Review 5.  Drugs versus bugs: in pursuit of the persistent predator Mycobacterium tuberculosis.

Authors:  James C Sacchettini; Eric J Rubin; Joel S Freundlich
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Authors:  J Zou; B M Hallberg; T Bergfors; F Oesch; M Arand; S L Mowbray; T A Jones
Journal:  Structure       Date:  2000-02-15       Impact factor: 5.006

7.  Cress and potato soluble epoxide hydrolases: purification, biochemical characterization, and comparison to mammalian enzymes.

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Review 9.  High throughput crystallography of TB drug targets.

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10.  Orally bioavailable potent soluble epoxide hydrolase inhibitors.

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Journal:  Biochimie       Date:  2012-06-18       Impact factor: 4.079

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3.  A self-compartmentalizing hexamer serine protease from Pyrococcus horikoshii: substrate selection achieved through multimerization.

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4.  The molecular structure of an epoxide hydrolase from Trichoderma reesei in complex with urea or amide-based inhibitors.

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5.  The structure-activity relationship of urea derivatives as anti-tuberculosis agents.

Authors:  Joshua R Brown; Elton J North; Julian G Hurdle; Christophe Morisseau; Jerrod S Scarborough; Dianqing Sun; Jana Korduláková; Michael S Scherman; Victoria Jones; Anna Grzegorzewicz; Rebecca M Crew; Mary Jackson; Michael R McNeil; Richard E Lee
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6.  Elevated faecal 12,13-diHOME concentration in neonates at high risk for asthma is produced by gut bacteria and impedes immune tolerance.

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7.  Drug Degradation Caused by mce3R Mutations Confers Contezolid (MRX-I) Resistance in Mycobacterium tuberculosis.

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8.  Design, synthesis and anti-tuberculosis activity of 1-adamantyl-3-heteroaryl ureas with improved in vitro pharmacokinetic properties.

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Journal:  Bioorg Med Chem       Date:  2013-02-26       Impact factor: 3.641

9.  Exported Epoxide Hydrolases Modulate Erythrocyte Vasoactive Lipids during Plasmodium falciparum Infection.

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Review 10.  Gates of enzymes.

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