Literature DB >> 9367777

Crystallization, structural determination and analysis of a novel parasite vaccine candidate: Fasciola hepatica glutathione S-transferase.

J Rossjohn1, S C Feil, M C Wilce, J L Sexton, T W Spithill, M W Parker.   

Abstract

Glutathione S-transferases (GSTs) represent the major class of detoxifying enzymes from parasitic helminths. As a result, they are candidates for chemotherapeutic and vaccine design. Indeed, GSTs from Fasciola hepatica have been found to be effective for vaccinating sheep and cattle against fasciolosis. This helminth contains at least seven GST isoforms, of which four have been cloned. The cloned isoforms (Fh51, Fh47, Fh7 and Fh1) all belong to the mu class of GSTs, share greater than 71% sequence identity, yet display distinct substrate specificities. Crystals of Fh47 were obtained using the hanging drop vapour diffusion technique. The crystals belong to space group I4122, with one monomer in the asymmetric unit, which corresponds to a very high solvent content of approximately 75%. The physiological dimer is generated via a crystallographic 2-fold rotation. The three-dimensional structure of Fh47 was solved by molecular replacement using the Schistosoma japonicum glutathione S-transferase (Sj26) crystal structure as a search model. The structure adopts the canonical GST fold comprising two domains: an N-terminal glutathione-binding domain, consisting of a four-stranded beta-sheet and three helices whilst the C-terminal domain is entirely alpha-helical. The presence of Phe19 in Fh47 results in a 6 degrees interdomain rotation in comparison to Sj26, where the equivalent residue is a leucine. Homology models of Fh51, Fh7 and Fh1, based on the Fh47 crystal structure, reveal critical differences in the residues lining the xenobiotic binding site, particularly at residue positions 9, 106 and 204. In addition, differences amongst the isoforms in the non-substrate binding site were noted, which may explain the observed differential binding of large ligands. The major immunogenic epitopes of Fh47 were surprisingly found not to reside on the most solvent-exposed regions of the molecule. Copyright 1997 Academic Press Limited

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Year:  1997        PMID: 9367777     DOI: 10.1006/jmbi.1997.1338

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


  14 in total

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3.  Mutagenic analysis of conserved arginine residues in and around the novel sulfate binding pocket of the human Theta class glutathione transferase T2-2.

Authors:  J U Flanagan; J Rossjohn; M W Parker; P G Board; G Chelvanayagam
Journal:  Protein Sci       Date:  1999-10       Impact factor: 6.725

Review 4.  Structure, function and evolution of glutathione transferases: implications for classification of non-mammalian members of an ancient enzyme superfamily.

Authors:  D Sheehan; G Meade; V M Foley; C A Dowd
Journal:  Biochem J       Date:  2001-11-15       Impact factor: 3.857

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Journal:  Parasitol Res       Date:  2007-07-20       Impact factor: 2.289

6.  Comparative assessment of recombinant and native immunogenic forms of Fasciola hepatica proteins for serodiagnosis of sheep fasciolosis.

Authors:  Kobra Mokhtarian; Ahmad Reza Meamar; Majid Khoshmirsafa; Elham Razmjou; Leila Masoori; Majid Khanmohammadi; Lame Akhlaghi; Reza Falak
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7.  A functionally conserved basic residue in glutathione transferases interacts with the glycine moiety of glutathione and is pivotal for enzyme catalysis.

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Journal:  Biochem J       Date:  2007-09-01       Impact factor: 3.857

8.  Assessment of Fasciola hepatica glutathione S-transferase as an antigen for serodiagnosis of human chronic fascioliasis.

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Journal:  Acta Trop       Date:  2018-07-07       Impact factor: 3.112

9.  Anthelmintics Resistance; How to Overcome it?

Authors:  Hatem A Shalaby
Journal:  Iran J Parasitol       Date:  2013-01       Impact factor: 1.012

10.  Differential activation of diverse glutathione transferases of Clonorchis sinensis in response to the host bile and oxidative stressors.

Authors:  Young-An Bae; Do-Whan Ahn; Eung-Goo Lee; Seon-Hee Kim; Guo-Bin Cai; Insug Kang; Woon-Mok Sohn; Yoon Kong
Journal:  PLoS Negl Trop Dis       Date:  2013-05-16
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