Mechanism of Thiol-Supported Arsenate Reduction Mediated by Phosphorolytic-Arsenolytic Enzymes: I. The Role of Arsenolysis

doi:10.1093/toxsci/kfp112

ToxSci Advance Access originally published online on May 27, 2009
Toxicological Sciences 2009 110(2):270-281; doi:10.1093/toxsci/kfp112

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Mechanism of Thiol-Supported Arsenate Reduction Mediated by Phosphorolytic-Arsenolytic Enzymes

I. The Role of Arsenolysis

Balázs Németi and Zoltán Gregus¹

Department of Pharmacology and Pharmacotherapy, Toxicology Section, University of Pécs, Medical School, Pécs 7624, Hungary

¹ To whom correspondence should be addressed at Department of Pharmacology and Pharmacotherapy, Toxicology Section, University of Pécs, Medical School, Szigeti út 12, H-7624 Pécs, Hungary. Fax: +36-72-536-218. E-mail: zoltan.gregus{at}aok.pte.hu.

Received March 25, 2009; accepted May 15, 2009

Abstract

Several mammalian enzymes catalyzing the phosphorolytic-arsenolyticcleavage of their substrates (thus yielding arsenylated metabolites)have been shown to facilitate reduction of arsenate (AsV) tothe more toxic arsenite (AsIII) in presence of their substrateand a thiol. These include purine nucleoside phosphorylase (PNP),glyceraldehyde-3-phosphate dehydrogenase (GAPDH), and glycogenphosphorylase-a (GPa). In this work, we tested further enzymes,the bacterial phosphotransacetylases (PTAs) and PNP, for AsVreduction. The PTAs, which arsenolytically cleave acetyl-CoAproducing acetyl-arsenate, were compared with GAPDH, which canalso form acetyl-arsenate by arsenolysis of its nonphysiologicalsubstrate, acetyl-phosphate. As these enzymes also mediatedAsV reduction, we can assert that facilitation of thiol-dependentAsV reduction may be a general property of enzymes that catalyzephosphorolytic-arsenolytic reactions. Because with all suchenzymes arsenolysis is obligatory for AsV reduction, we analyzedthe relationship between these two processes in presence ofvarious thiol compounds, using PNP. Although no thiol influencedthe rate of PNP-catalyzed arsenolysis, all enhanced the PNP-mediatedAsV reduction, albeit differentially. Furthermore, the relativecapacity of thiols to support AsV reduction mediated by PNP,GPa, PTA, and GAPDH apparently depended on the type of arsenylatedmetabolites (i.e., arsenate ester or anhydride) produced bythese enzymes. Importantly, AsV reduction by both acetyl-arsenate–producingenzymes (i.e., PTA and GAPDH) exhibited striking similaritiesin responsiveness to various thiols, thus highlighting the roleof arsenylated metabolite formation. This observation, togetherwith the finding that PNP-mediated AsV reduction lags behindthe PNP-catalyzed arsenolysis lead to the hypothesis that arsenolyticenzymes promote reduction of AsV by forming arsenylated metaboliteswhich are more reducible to AsIII by thiols than inorganic AsV.This hypothesis is evaluated in the adjoining paper.

Key Words: arsenate; reduction; thiols; glutathione; arsenolysis.

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