Glutathione-dependent activities of Trypanosoma cruzi p52 makes it a new member of the thiol:disulphide oxidoreductase family

Author:

MOUTIEZ Mireille1,QUÉMÉNEUR Eric2,SERGHERAERT Christian1,LUCAS Valérie1,TARTAR André1,DAVIOUD-CHARVET Elisabeth1

Affiliation:

1. Service de Chimie des biomolécules, URA CNRS 1309, Institut Pasteur de Lille, 1 rue du Pr Calmette, 59019 Lille, France

2. Département d'ingénierie et d'études des protéines, CEA, Bât. 152, CE Saclay, 91191 Gif-sur-yvette Cedex, France

Abstract

Trypanothione:glutathione disulphide thioltransferase of Trypanosoma cruzi (p52) is a key enzyme in the regulation of the intracellular thiolŐdisulphide redox balance by reducing glutathione disulphide. Here we show that p52, like other disulphide oxidoreductases possessing the CXXC active site motif, catalyses the reduction of low-molecular-mass disulphides (hydroxyethyldisulphide) as well as protein disulphides (insulin). However, p52 seems to be a poor oxidase under physiological conditions as evidenced by its very low rate for oxidative renaturation of reduced ribonuclease A. Like thioltransferase and protein disulphide isomerase, p52 was found to possess a glutathione-dependent dehydroascorbate reductase activity. The kinetic parameters were in the same range as those determined for mammalian dehydroascorbate reductases. A catalytic mechanism taking into account both trypanothione- and glutathione-dependent reduction reactions was proposed. This newly characterized enzyme is specific for the parasite and provides a new target for specific chemotherapy.

Publisher

Portland Press Ltd.

Subject

Cell Biology,Molecular Biology,Biochemistry

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