Literature DB >> 21630672

Investigations of the catalytic mechanism of thioredoxin glutathione reductase from Schistosoma mansoni.

Hsin-Hung Huang1, Latasha Day, Cynthia L Cass, David P Ballou, Charles H Williams, David L Williams.   

Abstract

Thioredoxin glutathione reductase from Schistosoma mansoni (SmTGR) catalyzes the reduction of both thioredoxin and glutathione disulfides (GSSG), thus playing a crucial role in maintaining redox homeostasis in the parasite. In line with this role, previous studies have demonstrated that SmTGR is a promising drug target for schistosomiasis. To aid in the development of efficacious drugs that target SmTGR, it is essential to understand the catalytic mechanism of SmTGR. SmTGR is a dimeric flavoprotein in the glutathione reductase family and has a head-to-tail arrangement of its monomers; each subunit has the components of both a thioredoxin reductase (TrxR) domain and a glutaredoxin (Grx) domain. However, the active site of the TrxR domain is composed of residues from both subunits: FAD and a redox-active Cys-154/Cys-159 pair from one subunit and a redox-active Cys-596'/Sec-597' pair from the other; the active site of the Grx domain contains a redox-active Cys-28/Cys-31 pair. Via its Cys-28/Cys-31 dithiol and/or its Cys-596'/Sec-597' thiol-selenolate, SmTGR can catalyze the reduction of a variety of substrates by NADPH. It is presumed that SmTGR catalyzes deglutathionylation reactions via the Cys-28/Cys-31 dithiol. Our anaerobic titration data suggest that reducing equivalents from NADPH can indeed reach the Cys-28/Cys-31 disulfide in the Grx domain to facilitate reductions effected by this cysteine pair. To clarify the specific chemical roles of each redox-active residue with respect to its various reactivities, we generated variants of SmTGR. Cys-28 variants had no Grx deglutathionylation activity, whereas Cys-31 variants retained partial Grx deglutathionylation activity, indicating that the Cys-28 thiolate is the nucleophile initiating deglutathionylation. Lags in the steady-state kinetics, found when wild-type SmTGR was incubated at high concentrations of GSSG, were not present in Grx variants, indicating that this cysteine pair is in some way responsible for the lags. A Sec-597 variant was still able to reduce a variety of substrates, albeit slowly, showing that selenocysteine is important but is not the sole determinant for the broad substrate tolerance of the enzyme. Our data show that Cys-520 and Cys-574 are not likely to be involved in the catalytic mechanism.

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Year:  2011        PMID: 21630672      PMCID: PMC3658134          DOI: 10.1021/bi200107n

Source DB:  PubMed          Journal:  Biochemistry        ISSN: 0006-2960            Impact factor:   3.162


  70 in total

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5.  A 1,536-well-based kinetic HTS assay for inhibitors of Schistosoma mansoni thioredoxin glutathione reductase.

Authors:  Wendy A Lea; Ajit Jadhav; Ganesha Rai; Ahmed A Sayed; Cynthia L Cass; James Inglese; David L Williams; Christopher P Austin; Anton Simeonov
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6.  Kinetic and mechanistic characterization and versatile catalytic properties of mammalian glutaredoxin 2: implications for intracellular roles.

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8.  Acid-base catalysis in the mechanism of thioredoxin reductase from Drosophila melanogaster.

Authors:  Hsin-Hung Huang; L David Arscott; David P Ballou; Charles H Williams
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9.  Platyhelminth mitochondrial and cytosolic redox homeostasis is controlled by a single thioredoxin glutathione reductase and dependent on selenium and glutathione.

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10.  Aurothioglucose inhibits murine thioredoxin reductase activity in vivo.

Authors:  A D Smith; C A Guidry; V C Morris; O A Levander
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Review 3.  The redox biology of schistosome parasites and applications for drug development.

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4.  Characterization of Lead Compounds Targeting the Selenoprotein Thioredoxin Glutathione Reductase for Treatment of Schistosomiasis.

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Review 6.  Thioredoxin glutathione reductase: its role in redox biology and potential as a target for drugs against neglected diseases.

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Review 7.  Thioredoxin glutathione reductase-dependent redox networks in platyhelminth parasites.

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8.  Discovery of New Anti-Schistosomal Hits by Integration of QSAR-Based Virtual Screening and High Content Screening.

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9.  Probing the Surface of a Parasite Drug Target Thioredoxin Glutathione Reductase Using Small Molecule Fragments.

Authors:  Francesca Fata; Ilaria Silvestri; Matteo Ardini; Rodolfo Ippoliti; Luana Di Leandro; Nicola Demitri; Maurizio Polentarutti; Adele Di Matteo; Haining Lyu; Gregory R J Thatcher; Pavel A Petukhov; David L Williams; Francesco Angelucci
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10.  Structural analysis of glutaredoxin domain of Mus musculus thioredoxin glutathione reductase.

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