4.6 Article

Methylation and demethylation of intermediates selenide and methylselenol in the metabolism of selenium

Journal

TOXICOLOGY AND APPLIED PHARMACOLOGY
Volume 226, Issue 2, Pages 169-177

Publisher

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.taap.2007.09.011

Keywords

demethylation; dimethylselenide; dimethylselenoxide; methylation; methylseleninic acid; methylselenocysteine; methylselenol; methyltransferase; selenide; selenium; trimethylselenonium

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All nutritional selenium sources are transformed into the assumed common intermediate selenide for the syntheses of selenoproteins for utilization and/or of selenosugar for excretion. Methylselenol [monomethylselenide, MMSe] is the assumed intermediate leading to other methylated metabolites, dimethylselenide (DMSe) and trimethylselenonium (TMSe) for excretion, and also to the intermediate selenide from methylselenocysteine and methylseleninic acid (MSA). Here, related methylation and demethylation reactions were studied in vitro by providing chemically reactive starting substrates (Se-76-selenide, (77) Se-MMSe and Se-82-DMSe) which were prepared in situ by the reduction of the corresponding labeled proximate precursors (Se-76-selenite, Se-77-MSA and Se-82-dimethylselenoxide (DMSeO), respectively) with glutathione, the three substrates being incubated simultaneously in rat organ supernatants and homogenates. The resulting chemically labile reaction products were detected simultaneously by speciation analysis with HPLC-ICP-MS after converting the products and un-reacted substrates to the corresponding oxidized derivatives (selenite, MSA and DMSeO). The time-related changes in selenium isotope profiles showed that demethylation of MMSe to selenide was efficient but that of DMSe to MMSe was negligible, whereas methylation of selenide to MMSe, and MMSe to DMSe were efficient, and that of DMSe to TMSe occurred less efficiently. The present methylation and demethylation reactions on equilibrium between selenide, MMSe and DMSe without producing selenosugar and selenoproteins indicated that DMSe rather than TMSe is produced as the end product, suggesting that DMSe is to be excreted more abundantly than TMSe. Organ-dependent differences in the methylation and demethylation reactions were characterized for the liver, kidney and lung. (c) 2007 Elsevier Inc. All rights reserved.

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