| Literature DB >> 29444934 |
Mark A Duerr1, Elisa N D Palladino1, Celine L Hartman1, James A Lambert2, Jacob D Franke1, Carolyn J Albert1, Sadis Matalon2, Rakesh P Patel3, Arne Slungaard4, David A Ford5.
Abstract
α-Chlorofatty aldehydes (α-ClFALDs) and α-bromofatty aldehydes (α-BrFALDs) are produced in activated neutrophils and eosinophils. This study investigated the ability of α-BrFALD and α-ClFALD to react with the thiols of GSH and protein cysteinyl residues. Initial studies showed that 2-bromohexadecanal (2-BrHDA) and 2-chlorohexadecanal (2-ClHDA) react with GSH producing the same fatty aldehyde-GSH adduct (FALD-GSH). In both synthetic and cellular reactions, FALD-GSH production was more robust with 2-BrHDA compared with 2-ClHDA as precursor. NaBr-supplemented phorbol myristate acetate (PMA)-activated neutrophils formed more α-BrFALD and FALD-GSH compared with non-NaBr-supplemented neutrophils. Primary human eosinophils, which preferentially produce hypobromous acid and α-BrFALD, accumulated FALD-GSH following PMA stimulation. Mice exposed to Br2 gas had increased levels of both α-BrFALD and FALD-GSH in the lungs, as well as elevated systemic plasma levels of FALD-GSH in comparison to mice exposed to air. Similar relative reactivity of α-ClFALD and α-BrFALD with protein thiols was shown using click analogs of these aldehydes. Collectively, these data demonstrate that GSH and protein adduct formation are much greater as a result of nucleophilic attack of cysteinyl residues on α-BrFALD compared with α-ClFALD, which was observed in both primary leukocytes and in mice exposed to bromine gas.Entities:
Keywords: fatty aldehydes; glutathione; hypobromous acid; hypochlorous acid; plasmalogen; thiols
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Year: 2018 PMID: 29444934 PMCID: PMC5880502 DOI: 10.1194/jlr.M083279
Source DB: PubMed Journal: J Lipid Res ISSN: 0022-2275 Impact factor: 5.922