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Literature DB >> 25346613

Quinone Methide Bioactivation Pathway: Contribution to Toxicity and/or Cytoprotection?

Abstract

The formation of quinone methides (QMs) from either direct 2-electron oxidation of 2- or 4-alkylphenols, isomerization of o-quinones, or elimination of a good leaving group could explain the cytotoxic/cytoprotective effects of several drugs, natural products, as well as endogenous compounds. For example, the antiretroviral drug nevirapine and the antidiabetic agent troglitazone both induce idiosyncratic hepatotoxicity through mechanisms involving quinone methide formation. The anesthetic phencyclidine induces psychological side effects potentially through quinone methide mediated covalent modification of crucial macromolecules in the brain. Selective estrogen receptor modulators (SERMs) such as tamoxifen, toremifene, and raloxifene are metabolized to quinone methides which could potentially contribute to endometrial carcinogenic properties and/or induce detoxification enzymes and enhance the chemopreventive effects of these SERMs. Endogenous estrogens and/or estrogens present in estrogen replacement formulations are also metabolized to catechols and further oxidized to o-quinones which can isomerize to quinone methides. Both estrogen quinoids could cause DNA damage which could enhance hormone dependent cancer risk. Natural products such as the food and flavor agent eugenol can be directly oxidized to a quinone methide which may explain the toxic effects of this natural compound. Oral toxicities associated with chewing areca quid could be the result of exposure to hydroxychavicol through initial oxidation to an o-quinone which isomerizes to a p-quinone methide. Similar o-quinone to p-quinone methide isomerization reactions have been reported for the ubiquitous flavonoid quercetin which needs to be taken into consideration when evaluating risk-benefit assessments of these natural products. The resulting reaction of these quinone methides with proteins, DNA, and/or resulting modulation of gene expression may explain the toxic and/or beneficial effects of the parent compounds.

Entities: CellLine Chemical Disease Gene Species

Keywords: P450; bioactivation; quinone; quinone methide; selective estrogen receptor modulators (SERMs)

Year: 2014 PMID： 25346613 PMCID： PMC4204646 DOI： 10.2174/138527281801140121123046

Source DB: PubMed Journal: Curr Org Chem ISSN： 1385-2728 Impact factor: 2.180

107 in total

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Authors: Muhammad Zahid; Ekta Kohli; Muhammad Saeed; Eleanor Rogan; Ercole Cavalieri
Journal: Chem Res Toxicol Date: 2006-01 Impact factor: 3.739

2. 4-Hydroxylated metabolites of the antiestrogens tamoxifen and toremifene are metabolized to unusually stable quinone methides.

Authors: P W Fan; F Zhang; J L Bolton
Journal: Chem Res Toxicol Date: 2000-01 Impact factor: 3.739

3. Investigation of the regio- and stereo-selectivity of deoxyguanosine linkage to deuterated 2-hydroxyestradiol by using liquid chromatography/ESI-ion trap mass spectrometry.

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Journal: J Am Soc Mass Spectrom Date: 2003-04 Impact factor: 3.109

4. Dietary quercetin glycosides: antioxidant activity and induction of the anticarcinogenic phase II marker enzyme quinone reductase in Hepalclc7 cells.

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Journal: Carcinogenesis Date: 1996-11 Impact factor: 4.944

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Journal: Pharmacol Ther Date: 1984 Impact factor: 12.310

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Journal: Mutat Res Date: 2005-03-31 Impact factor: 2.433

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Journal: Cancer Res Date: 1993-10-01 Impact factor: 12.701

9. Evidence that 4-allyl-o-quinones spontaneously rearrange to their more electrophilic quinone methides: potential bioactivation mechanism for the hepatocarcinogen safrole.

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Journal: Chem Res Toxicol Date: 1994 May-Jun Impact factor: 3.739

10. Bioactivation of the cancer chemopreventive agent tamoxifen to quinone methides by cytochrome P4502B6 and identification of the modified residue on the apoprotein.

Authors: Chitra Sridar; Jaime D'Agostino; Paul F Hollenberg
Journal: Drug Metab Dispos Date: 2012-08-31 Impact factor: 3.922

13 in total

1. Alcohol, Aldehyde, and Ketone Liberation and Intracellular Cargo Release through Peroxide-Mediated α-Boryl Ether Fragmentation.

Authors: Ramsey D Hanna; Yuta Naro; Alexander Deiters; Paul E Floreancig
Journal: J Am Chem Soc Date: 2016-09-30 Impact factor: 15.419

2. Ectopic suicide inhibition of thioredoxin glutathione reductase.

Authors: Ilaria Silvestri; Haining Lyu; Francesca Fata; Paul R Banta; Benedetta Mattei; Rodolfo Ippoliti; Andrea Bellelli; Giuseppina Pitari; Matteo Ardini; Valentina Petukhova; Gregory R J Thatcher; Pavel A Petukhov; David L Williams; Francesco Angelucci
Journal: Free Radic Biol Med Date: 2019-12-20 Impact factor: 7.376

3. Expression of Cyclooxygenase-2, Nitric Oxide Synthase 2 and Heme Oxygenase-1 mRNA Induced by Bis-Eugenol in RAW264.7 Cells and their Antioxidant Activity Determined Using the Induction Period Method.

Authors: Yukio Murakami; Akifumi Kawata; Seiichiro Fujisawa
Journal: In Vivo Date: 2017 Sep-Oct Impact factor: 2.155

4. Purple pigment from Peltogyne mexicana heartwood as a potential colorant for food.

Authors: Paulina Gutiérrez-Macías; Cinthya G Gutiérrez-Zúñiga; Leticia Garduño-Siciliano; Cynthia Ordaz-Pichardo; Myriam Arriaga-Alba; Blanca E Barragán-Huerta
Journal: J Food Sci Technol Date: 2019-06-06 Impact factor: 2.701

5. Targeting duplex DNA with the reversible reactivity of quinone methides.

Authors: Chengyun Huang; Yang Liu; Steven E Rokita
Journal: Signal Transduct Target Ther Date: 2016-06-24

Review 6. Compounds From Celastraceae Targeting Cancer Pathways and Their Potential Application in Head and Neck Squamous Cell Carcinoma: A Review.

Authors: Camila Hernandes; Ana Maria Soares Pereira; Patricia Severino
Journal: Curr Genomics Date: 2017-02 Impact factor: 2.236

10. Pharmacologic ATF6 activating compounds are metabolically activated to selectively modify endoplasmic reticulum proteins.

Authors: Ryan Paxman; Lars Plate; Erik A Blackwood; Chris Glembotski; Evan T Powers; R Luke Wiseman; Jeffery W Kelly
Journal: Elife Date: 2018-08-07 Impact factor: 8.140