Literature DB >> 11329271

Eosinophil peroxidase catalyzes bromination of free nucleosides and double-stranded DNA.

Z Shen1, S N Mitra, W Wu, Y Chen, Y Yang, J Qin, S L Hazen.   

Abstract

Chronic parasitic infections are a major risk factor for cancer development in many underdeveloped countries. Oxidative damage of DNA may provide a mechanism linking these processes. Eosinophil recruitment is a hallmark of parasitic infections and many forms of cancer, and eosinophil peroxidase (EPO), a secreted hemoprotein, plays a central role in oxidant production by these cells. However, mechanisms through which EPO may facilitate DNA oxidation have not been fully characterized. Here, we show that EPO effectively uses plasma levels of bromide as a cosubstrate to brominate bases in nucleotides and double-stranded DNA, forming several stable novel brominated adducts. Products were characterized by HPLC with on-line UV spectroscopy and electrospray ionization tandem mass spectrometry (LC/ESI/MS/MS). Ring assignments for brominated purine bases as their 8-bromo adducts were identified by NMR spectroscopy. Using stable isotope dilution LC/ESI/MS/MS, we show that while guanine is the preferred purine targeted for bromination as a free nucleobase, 8-bromoadenine is the major purine oxidation product generated following exposure of double-stranded DNA to either HOBr or the EPO/H(2)O(2)/Br(-) system. Bromination of nucleobases was inhibited by scavengers of hypohalous acids such as the thioether methionine, but not by a large molar excess of primary amines. Subsequently, N-monobromoamines were demonstrated to be effective brominating agents for both free nucleobases and adenine within intact DNA. A rationale for selective modification of adenine, but not guanine, in double-stranded DNA based upon stereochemical criteria is presented. Collectively, these results suggest that specific brominated DNA bases may serve as novel markers for monitoring oxidative damage of DNA and the nucleotide pool by brominating oxidants.

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Year:  2001        PMID: 11329271     DOI: 10.1021/bi001961t

Source DB:  PubMed          Journal:  Biochemistry        ISSN: 0006-2960            Impact factor:   3.162


  10 in total

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2.  Halogen bonds in biological molecules.

Authors:  Pascal Auffinger; Franklin A Hays; Eric Westhof; P Shing Ho
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4.  Identification of dihalogenated proteins in rat intestinal mucosa injured by indomethacin.

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5.  Myeloperoxidase-derived oxidation: mechanisms of biological damage and its prevention.

Authors:  Michael J Davies
Journal:  J Clin Biochem Nutr       Date:  2010-12-28       Impact factor: 3.114

6.  Stability of 3-bromotyrosine in serum and serum 3-bromotyrosine concentrations in dogs with gastrointestinal diseases.

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7.  Dual binding mode of antithyroid drug methimazole to mammalian heme peroxidases - structural determination of the lactoperoxidase-methimazole complex at 1.97 Å resolution.

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8.  Mutagenic consequences of cytosine alterations site-specifically embedded in the human genome.

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9.  Mutation Spectrum Induced by 8-Bromoguanine, a Base Damaged by Reactive Brominating Species, in Human Cells.

Authors:  Kazuya Shinmura; Hisami Kato; Masanori Goto; Hong Tao; Yusuke Inoue; Satoki Nakamura; Haruki Yoshida; Emi Tsuzaki; Haruhiko Sugimura
Journal:  Oxid Med Cell Longev       Date:  2017-09-30       Impact factor: 6.543

10.  Eosinophil peroxidase over-expression predicts the clinical outcome of patients with primary lung adenocarcinoma.

Authors:  Liang Ye; Hongying Wang; Huijuan Li; Hongbing Liu; Tangfeng Lv; Yong Song; Fang Zhang
Journal:  J Cancer       Date:  2019-01-29       Impact factor: 4.207

  10 in total

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