FEBS Letters
Volume 581, Issue 19 , Pages 3598-3607, 31 July 2007

The system biology of thiol redox system in Escherichia coli and yeast: Differential functions in oxidative stress, iron metabolism and DNA synthesis

Edited by Roberto Sitia

CEA, iBiTecS, Laboratoire Stress Oxydants et Cancer, Gif sur Yvette F-91191, France

Received 11 June 2007; accepted 2 July 2007. published online 11 July 2007.

Abstract 

By its ability to engage in a variety of redox reactions and coordinating metals, cysteine serves as a key residue in mediating enzymatic catalysis, protein oxidative folding and trafficking, and redox signaling. The thiol redox system, which consists of the glutathione and thioredoxin pathways, uses the cysteine residue to catalyze thiol-disulfide exchange reactions, thereby controlling the redox state of cytoplasmic cysteine residues and regulating the biological functions it subserves. Here, we consider the thiol redox systems of Escherichia coli and Saccharomyces cerevisiae, emphasizing the role of genetic approaches in the understanding of the cellular functions of these systems. We show that although prokaryotic and eukaryotic systems have a similar architecture, they profoundly differ in their overall cellular functions.

Keywords: Thiol redox control, Thioredoxin, Glutathione, Oxidative stress, Iron metabolism, Ribonucleotide reductase

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PII: S0014-5793(07)00755-7

doi:10.1016/j.febslet.2007.07.002

Refers to corrigendum:

  • Corrigendum to “The system biology of thiol redox system in Escherichia coli and yeast: Differential functions in oxidative stress, iron metabolism and DNA synthesis” [FEBS Lett. 581 (2007) 3598–3607] , 08 August 2007

    Michel B. Toledano, Chitranshu Kumar, Natacha Le Moan, Dan Spector, Frédérique Tacnet
    FEBS Letters 18 September 2007 (Vol. 581, Issue 23, Page 4549)

FEBS Letters
Volume 581, Issue 19 , Pages 3598-3607, 31 July 2007