Thiol Redox Sensitivity of Two Key Enzymes of Heme Biosynthesis and Pentose Phosphate Pathways: Uroporphyrinogen Decarboxylase and Transketolase

Author:

McDonagh Brian12ORCID,Pedrajas José Rafael3,Padilla C. Alicia1,Bárcena José Antonio1

Affiliation:

1. Department of Biochemistry and Molecular Biology, University of Córdoba and Córdoba Maimónides Institute for Biomedical Research (IMIBIC), 14071 Córdoba, Spain

2. Department of Musculoskeletal Biology, Institute of Ageing and Chronic Disease (IACD), University of Liverpool, Liverpool L69 3GA, UK

3. Molecular Signaling and Antioxidant Systems in Plants, Department of Experimental Biology, University of Jaén, 23071 Jaén, Spain

Abstract

Uroporphyrinogen decarboxylase (Hem12p) and transketolase (Tkl1p) are key mediators of two critical processes within the cell, heme biosynthesis, and the nonoxidative part of the pentose phosphate pathway (PPP). The redox properties of both Hem12p and Tkl1p fromSaccharomyces cerevisiaewere investigated using proteomic techniques (SRM and label-free quantification) and biochemical assays in cell extracts andin vitrowith recombinant proteins. Thein vivoanalysis revealed an increase in oxidized Cys-peptides in the absence of Grx2p, and also after treatment with H2O2in the case of Tkl1p, without corresponding changes in total protein, demonstrating a true redox response. Out of three detectable Cys residues in Hem12p, only the conserved residue Cys52 could be modified by glutathione and efficiently deglutathionylated by Grx2p, suggesting a possible redox control mechanism for heme biosynthesis. On the other hand, Tkl1p activity was sensitive to thiol redox modification and although Cys622 could be glutathionylated to a limited extent, it was not a natural substrate of Grx2p. The human orthologues of both enzymes have been involved in certain cancers and possess Cys residues equivalent to those identified as redox sensitive in yeast. The possible implication for redox regulation in the context of tumour progression is put forward.

Funder

Andalusian Government

Publisher

Hindawi Limited

Subject

Cell Biology,Ageing,General Medicine,Biochemistry

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