Literature DB >> 15962938

Formation of 8-oxo-7,8-dihydro-2'-deoxyguanosine (8-oxo-dGuo) by PAH o-quinones: involvement of reactive oxygen species and copper(II)/copper(I) redox cycling.

Jong-Heum Park1, Sridhar Gopishetty, Lawrence M Szewczuk, Andrea B Troxel, Ronald G Harvey, Trevor M Penning.   

Abstract

Polycyclic aromatic hydrocarbons (PAHs) are ubiquitous environmental pollutants and procarcinogens that require activation by host metabolism. Metabolic activation of PAHs by aldo-keto reductases (AKRs) leads to formation of reactive and redox active o-quinones, which may cause oxidatively generated DNA damage. Spectrophotometric assays showed that NADPH caused PAH o-quinones to enter futile redox cycles, which result in the depletion of excess cofactor. Copper(II) amplified NADPH-dependent redox cycling of the o-quinones. Concurrent with NADPH oxidation, molecular oxygen was consumed, indicating the production of ROS. To determine whether PAH o-quinones can cause 8-oxo-dGuo formation in salmon testis DNA, three prerequisite experimental conditions were satisfied. Quantitative complete enzymatic hydrolysis of DNA was achieved, adventitious oxidation of dGuo was eliminated by the use of chelex and desferal, and basal levels of less than 2.0 8-oxo-dGuo/10(5) dGuo were obtained. The HPLC-ECD analytical method was validated by spiking the DNA with standard 8-oxo-dGuo and demonstrating quantitative recovery. HPLC-ECD analysis revealed that in the presence of NADPH and Cu(II), submicromolar concentrations of PAH o-quinones generated >60.0 8-oxo-dGuo adducts/10(5) dGuo. The rank order of 8-oxo-dGuo generated in isolated DNA was NP-1,2-dione > BA-3,4-dione > 7,12-DMBA-3,4-dione > BP-7,8-dione. The formation of 8-oxo-dGuo by PAH o-quinones was concentration-dependent. It was completely or partially inhibited when catalase, tiron, or a Cu(I) specific chelator, bathocuproine, was added, indicating the requirement for H(2)O(2), O(2)(-), and Cu(I), respectively. Methional, which is a copper-hydroperoxo complex [Cu(I)OOH] scavenger, also suppressed 8-oxo-dGuo formation. By contrast, mannitol, sodium benzoate, and sodium formate, which act as hydroxyl radical scavengers, did not block its formation. Sodium azide, which can act as both a hydroxyl radical and a (1)O(2) scavenger, abolished the formation of 8-oxo-dGuo. These data showed that the production of 8-oxo-dGuo was dependent on Cu(II)/Cu(I) catalyzed redox cycling of PAH o-quinones to produce ROS and that the immediate oxidant was not hydroxyl radical or Cu(I)OOH and that it is more likely (1)O(2), which can produce a 4,8-endoperoxide-dGuo intermediate.

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Year:  2005        PMID: 15962938      PMCID: PMC1314988          DOI: 10.1021/tx050001a

Source DB:  PubMed          Journal:  Chem Res Toxicol        ISSN: 0893-228X            Impact factor:   3.739


  48 in total

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Authors:  H Wei; Q Cai; R Rahn; X Zhang
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2.  The reaction of (+/-)-7alpha, 8beta-dihydroxy-9beta, 10beta-epoxy-7,8,9,10-tetrahydrobenzo(a)pyrene with DNA.

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3.  Activation of c-Ha-ras-1 proto-oncogene by in vitro modification with a chemical carcinogen, benzo(a)pyrene diol-epoxide.

Authors:  C J Marshall; K H Vousden; D H Phillips
Journal:  Nature       Date:  1984 Aug 16-22       Impact factor: 49.962

4.  Binding of benzo[a]pyrene 7,8-diol-9,10-epoxides to DNA, RNA, and protein of mouse skin occurs with high stereoselectivity.

Authors:  M Koreeda; P D Moore; P G Wislocki; W Levin; H Yagi; D M Jerina
Journal:  Science       Date:  1978-02-17       Impact factor: 47.728

5.  Preferential formation of benzo[a]pyrene adducts at lung cancer mutational hotspots in P53.

Authors:  M F Denissenko; A Pao; M Tang; G P Pfeifer
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6.  Spectroscopic identification of ortho-quinones as the products of polycyclic aromatic trans-dihydrodiol oxidation catalyzed by dihydrodiol dehydrogenase. A potential route of proximate carcinogen metabolism.

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8.  Partitioning of zinc and copper within subnuclear nucleoprotein particles.

Authors:  S E Bryan; D L Vizard; D A Beary; R A LaBiche; K J Hardy
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9.  Oxidative DNA damage induced by benz[a]anthracene dihydrodiols in the presence of dihydrodiol dehydrogenase.

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Journal:  Chem Res Toxicol       Date:  2004-11       Impact factor: 3.739

10.  Singlet oxygen-induced mutations in M13 lacZ phage DNA.

Authors:  D Decuyper-Debergh; J Piette; A Van de Vorst
Journal:  EMBO J       Date:  1987-10       Impact factor: 11.598

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  28 in total

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2.  Oxidatively generated DNA damage after Cu(II) catalysis of dopamine and related catecholamine neurotransmitters and neurotoxins: Role of reactive oxygen species.

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3.  HPLC Measurement of the DNA Oxidation Biomarker, 8-oxo-7,8-dihydro-2'-deoxyguanosine, in Cultured Cells and Animal Tissues.

Authors:  Nikolai L Chepelev; Dean A Kennedy; Remi Gagné; Taryn White; Alexandra S Long; Carole L Yauk; Paul A White
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4.  Comparison of p53 mutations induced by PAH o-quinones with those caused by anti-benzo[a]pyrene diol epoxide in vitro: role of reactive oxygen and biological selection.

Authors:  Yu-Min Shen; Andrea B Troxel; Srilakshmi Vedantam; Trevor M Penning; Jeffrey Field
Journal:  Chem Res Toxicol       Date:  2006-11       Impact factor: 3.739

5.  Specificity of human aldo-keto reductases, NAD(P)H:quinone oxidoreductase, and carbonyl reductases to redox-cycle polycyclic aromatic hydrocarbon diones and 4-hydroxyequilenin-o-quinone.

Authors:  Carol A Shultz; Amy M Quinn; Jong-Heum Park; Ronald G Harvey; Judy L Bolton; Edmund Maser; Trevor M Penning
Journal:  Chem Res Toxicol       Date:  2011-09-29       Impact factor: 3.739

6.  Different mechanisms between copper and iron in catecholamines-mediated oxidative DNA damage and disruption of gene expression in vitro.

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7.  Nrf transcription factors in keratinocytes are essential for skin tumor prevention but not for wound healing.

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9.  Protein lysine-Nζ alkylation and O-phosphorylation mediated by DTT-generated reactive oxygen species.

Authors:  Nigam Kumar; Hans Ippel; Christian Weber; Tilman Hackeng; Kevin H Mayo
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10.  Evidence for the aldo-keto reductase pathway of polycyclic aromatic trans-dihydrodiol activation in human lung A549 cells.

Authors:  Jong-Heum Park; Dipti Mangal; Kirk A Tacka; Amy M Quinn; Ronald G Harvey; Ian A Blair; Trevor M Penning
Journal:  Proc Natl Acad Sci U S A       Date:  2008-05-12       Impact factor: 11.205

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