Assessing dose-dependent differences in DNA-damage, p53 response and genotoxicity for quercetin and curcumin

被引:29
作者
Sun, Bin [1 ]
Ross, Susan M. [1 ]
Trask, O. Joseph [1 ]
Carmichael, Paul L. [2 ]
Dent, Matthew [2 ]
White, Andrew [2 ]
Andersen, Melvin E. [1 ]
Clewell, Rebecca A. [1 ]
机构
[1] Hamner Inst Hlth Sci, Res Triangle Pk, NC 27709 USA
[2] Unilever, Safety & Environm Assurance Ctr, Sharnbrook MK44 1LQ, Beds, England
关键词
DNA damage; Polyphenols; Micronucleus; p53; Quercetin; Curcumin; DNA repair; CELL-CYCLE ARREST; BREAST-CANCER CELLS; P53-DEPENDENT APOPTOSIS; FLAVONOID QUERCETIN; MICRONUCLEUS ASSAY; CARCINOMA-CELLS; HISTONE H2AX; INHIBITION; ACTIVATION; EXPRESSION;
D O I
10.1016/j.tiv.2013.05.015
中图分类号
R99 [毒物学(毒理学)];
学科分类号
100405 ;
摘要
As part of a longer-term goal to create a quantitative mechanistic model of the p53-Mdm2 DNA-damage pathway, we are studying cellular responses to compounds causing DNA-damage by various modes-of action, including two natural polyphenols: quercetin (QUE) and curcumin (CUR). QUE and CUR are weak mutagens in some in vitro assays and possess both anti- or pro-oxidant effects depending on dose. This study examines the dose-response of DNA-damage pathway to these compounds in HT1080 cells (a human cell line with wild-type p53) at doses relevant to human exposure. CUR was more potent in causing reactive oxygen species, DNA damage (measured as phospho-H2AX) and p53 induction, with lowest observed effect levels (LOELs; 3-8 mu M) approximately three-fold lower than QUE (20-30 mu M). CUR showed a strong G2/M arrest and apoptosis at similar to 10 mu M. QUE caused S phase arrest at low doses (8 mu M) and apoptosis was only induced at much higher doses (60 mu M). At concentrations with similar levels of p-H2AX and p53 biomarkers, CUR caused greater micronuclei frequency. CUR induced clear increases micronuclei at 3-6 mu M, while QUE had a weaker micronuclei response even at the highest doses. Thus, even with two compounds sharing common chemistries, DNA-damage response patterns differed significantly in terms of dose and cell fate. (c) 2013 Elsevier Ltd. All rights reserved.
引用
收藏
页码:1877 / 1887
页数:11
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