| Literature DB >> 24974182 |
Danyelle M Townsend1, Volodymyr I Lushchak2, Arthur J L Cooper3.
Abstract
Glutathionylation is generally a reversible posttranslational modification that occurs to cysteine residues that have been exposed to reactive oxygen species (P-SSG). This cyclical process can regulate various clusters of proteins, including those involved in critical cellular signaling functions. However, certain conditions can favor the formation of dehydroamino acids, such as 2,3-didehydroalanine (2,3-dehydroalanine, DHA) and 2,3-didehydrobutyrine (2,3-dehydrobutyrine), which can act as Michael acceptors. In turn, these can form Michael adducts with glutathione (GSH), resulting in the formation of a stable thioether conjugate, an irreversible process referred to as nonreducible glutathionylation. This is predicted to be prevalent in nature, particularly in more slowly turning over proteins. Such nonreducible glutathionylation can be distinguished from the more facile cycling signaling processes and is predicted to be of gerontological, toxicological, pharmacological, and oncological relevance. Here, we compare reversible and irreversible glutathionylation.Entities:
Keywords: Dehydroalanine; Glutaredoxin; Glutathione; Glutathione S-transferases; Glutathione disulfide; Irreversible protein glutathionylation; Lanthionine; Reversible glutathionylation; γ-Glutamyl-L-cysteine
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Year: 2014 PMID: 24974182 PMCID: PMC4603650 DOI: 10.1016/B978-0-12-420117-0.00005-0
Source DB: PubMed Journal: Adv Cancer Res ISSN: 0065-230X Impact factor: 6.242