Literature DB >> 22498038

Genotoxicity of the cancer chemopreventive drug candidates CP-31398, SHetA2, and phospho-ibuprofen.

Rupa S Doppalapudi1, Edward S Riccio, Zoe Davis, Sean Menda, Abraham Wang, Nicholas Du, Carol Green, Levy Kopelovich, Chinthalapally V Rao, Doris M Benbrook, Izet M Kapetanovic.   

Abstract

The genotoxic activities of three cancer chemopreventive drug candidates, CP-31398 (a cell permeable styrylquinazoline p53 modulator), SHetA2 (a flexible heteroarotinoid), and phospho-ibuprofen (PI, a derivative of ibuprofen) were tested. None of the compounds were mutagenic in the Salmonella/Escherichia coli/microsome plate incorporation test. CP-31398 and SHetA2 did not induce chromosomal aberrations (CA) in Chinese hamster ovary (CHO) cells, either in the presence or absence of rat hepatic S9 (S9). PI induced CA in CHO cells, but only in the presence of S9. PI, its parent compound ibuprofen, and its moiety diethoxyphosphoryloxybutyl alcohol (DEPBA) were tested for CA and micronuclei (MN) in CHO cells in the presence of S9. PI induced CA as well as MN, both kinetochore-positive (Kin+) and -negative (Kin-), in the presence of S9 at ≤100μg/ml. Ibuprofen was negative for CA, positive for MN with Kin+ at 250μg/ml, and positive for MN with Kin- at 125 and 250μg/ml. DEPBA induced neither CA nor MN at ≤5000μg/ml. The induction of chromosomal damage in PI-treated CHO cells in the presence of S9 may be due to its metabolites. None of the compounds were genotoxic, in the presence or absence of S9, in the GADD45α-GFP Human GreenScreen assay and none induced MN in mouse bone marrow erythrocytes.
Copyright © 2012 Elsevier B.V. All rights reserved.

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Year:  2012        PMID: 22498038      PMCID: PMC3375211          DOI: 10.1016/j.mrgentox.2012.03.009

Source DB:  PubMed          Journal:  Mutat Res        ISSN: 0027-5107            Impact factor:   2.433


  38 in total

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Journal:  Mutat Res       Date:  1975-02       Impact factor: 2.433

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Journal:  Mutat Res       Date:  1983-06       Impact factor: 2.433

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10.  CP-31398 restores DNA-binding activity to mutant p53 in vitro but does not affect p53 homologs p63 and p73.

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Journal:  J Biol Chem       Date:  2004-08-11       Impact factor: 5.157

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3.  Dose-dependent efficacy and safety toxicology of hydroxypyridinonate actinide decorporation agents in rodents: towards a safe and effective human dosing regimen.

Authors:  Deborah I Bunin; Polly Y Chang; Rupa S Doppalapudi; Edward S Riccio; Dahlia An; Erin E Jarvis; Birgitta Kullgren; Rebecca J Abergel
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4.  Vaginal Suppositories Containing SHetA2 to Treat Cervical Dysplasia: Pharmacokinetics of Daily Doses and Preliminary Safety Profile.

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5.  Physiologically Based Pharmacokinetic Modeling and Tissue Distribution Characteristics of SHetA2 in Tumor-Bearing Mice.

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6.  Pharmacokinetics and Pharmacodynamics of Escalating Doses of SHetA2 After Vaginal Administration to Mice.

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7.  SHetA2 interference with mortalin binding to p66shc and p53 identified using drug-conjugated magnetic microspheres.

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Journal:  Invest New Drugs       Date:  2013-11-20       Impact factor: 3.850

8.  Bioanalytical method development and validation of HPLCUV assay for the quantification of SHetA2 in mouse and human plasma: Application to pharmacokinetics study.

Authors:  Ankur Sharma; Elangovan Thavathiru; Doris Mangiaracina Benbrook; Sukyung Woo
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9.  Utility and Mechanism of SHetA2 and Paclitaxel for Treatment of Endometrial Cancer.

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10.  Pharmacokinetics and interspecies scaling of a novel, orally-bioavailable anti-cancer drug, SHetA2.

Authors:  Ankur Sharma; Doris Mangiaracina Benbrook; Sukyung Woo
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