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Structural and mechanistic insights into type II trypanosomatid tryparedoxin-dependent peroxidases

  作者 Alphey, MS; Konig, J; Fairlamb, AH  
  选自 期刊  Biochemical Journal;  卷期  2008年414-3;  页码  375-381  
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[摘要]TbTDPX (Trypanosoma brucei tryparedoxin-dependent peroxidase) is a genetically validated drug target in the fight against African sleeping sickness. Despite its similarity to members of the GPX (glutathione peroxidase) family, TbTDPX2 is functional as a monomer, lacks a selenocysteine residue and relies instead on peroxidatic and resolving cysteine residues for catalysis and uses tryparedoxin rather than glutathione as electron donor. Kinetic studies indicate a saturable Ping Pong mechanism, unlike selenium-dependent GPXs, which display infinite K-m and V-max values. The structure of the reduced enzyme at 2.1 angstrom (0.21 nm) resolution reveals that the catalytic thiol groups are widely separated [19 angstrom (0.19 nm)] and thus unable to form a disulphide bond without a large conformational change in the secondary-structure architecture, as reported for certain plant GPXs. A model of the oxidized enzyme structure is presented and the implications for small-molecule inhibition are discussed.

 
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