Literature DB >> 15238237

Genotoxicity of malachite green and leucomalachite green in female Big Blue B6C3F1 mice.

Roberta A Mittelstaedt1, Nan Mei, Peggy J Webb, Joseph G Shaddock, Vasily N Dobrovolsky, Lynda J McGarrity, Suzanne M Morris, Tao Chen, Frederick A Beland, Kevin J Greenlees, Robert H Heflich.   

Abstract

Malachite green, a triphenylmethane dye used in aquaculture as an antifungal agent, is rapidly reduced in vivo to leucomalachite green. Previous studies in which female B6C3F1 mice were fed malachite green produced relatively high levels of liver DNA adducts after 28 days, but no significant induction of liver tumors was detected in a 2-year feeding study. Comparable experiments conducted with leucomalachite green resulted in relatively low levels of liver DNA adducts but a dose-responsive induction of liver tumors. In the present study, we fed transgenic female Big Blue B6C3F1 mice with 450 ppm malachite green and 204 and 408 ppm leucomalachite green (the high doses used in the tumor bioassays) and evaluated genotoxicity after 4 and 16 weeks of treatment. Neither malachite green nor leucomalachite green increased the peripheral blood micronucleus frequency or Hprt lymphocyte mutant frequency at either time point; however, the 16-week treatment with 408 ppm leucomalachite green did increase the liver cII mutant frequency. Similar increases in liver cII mutant frequency were not seen in the mice treated for 16 weeks with malachite green or in female Big Blue rats treated with a comparable dose of leucomalachite green for 16 weeks in a previous study [Mutat. Res. 547 (2004) 5]. These results indicate that leucomalachite green is an in vivo mutagen in transgenic female mouse liver and that the mutagenicities of malachite green and leucomalachite green correlate with their tumorigenicities in mice and rats. The lack of increased micronucleus frequencies and lymphocyte Hprt mutants in female mice treated with leucomalachite green suggests that its genotoxicity is targeted to the tissue at risk for tumor induction.

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Year:  2004        PMID: 15238237     DOI: 10.1016/j.mrgentox.2004.04.003

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


  6 in total

1.  Investigating the Generalizability of the MultiFlow ® DNA Damage Assay and Several Companion Machine Learning Models With a Set of 103 Diverse Test Chemicals.

Authors:  Steven M Bryce; Derek T Bernacki; Stephanie L Smith-Roe; Kristine L Witt; Jeffrey C Bemis; Stephen D Dertinger
Journal:  Toxicol Sci       Date:  2018-03-01       Impact factor: 4.849

2.  Design and characterization of a direct ELISA for the detection and quantification of leucomalachite green.

Authors:  Gurmit Singh; Terence Koerner; Jean-Marc Gelinas; Michael Abbott; Beth Brady; Anne-Catherine Huet; Caroline Charlier; Philippe Delahaut; Samuel Benrejeb Godefroy
Journal:  Food Addit Contam Part A Chem Anal Control Expo Risk Assess       Date:  2011-06

3.  Rapid degradation of malachite green by CoFe2O4-SiC foam under microwave radiation.

Authors:  Yanpeng Mao; Shanxiu Yang; Chao Xue; Miaomiao Zhang; Wenlong Wang; Zhanlong Song; Xiqiang Zhao; Jing Sun
Journal:  R Soc Open Sci       Date:  2018-06-27       Impact factor: 2.963

4.  Triphenylmethane dye activation of beta-arrestin.

Authors:  Larry S Barak; Yushi Bai; Joshua C Snyder; Jiangbo Wang; Wei Chen; Marc G Caron
Journal:  Biochemistry       Date:  2013-08-01       Impact factor: 3.162

5.  Enhanced sensitive immunoassay: noncompetitive phage anti-immune complex assay for the determination of malachite green and leucomalachite green.

Authors:  Jie-Xian Dong; Chao Xu; Hong Wang; Zhi-Li Xiao; Shirley J Gee; Zhen-Feng Li; Feng Wang; Wei-Jian Wu; Yu-Dong Shen; Jin-Yi Yang; Yuan-Ming Sun; Bruce D Hammock
Journal:  J Agric Food Chem       Date:  2014-08-18       Impact factor: 5.279

Review 6.  Thresholds of Genotoxic and Non-Genotoxic Carcinogens.

Authors:  Takehiko Nohmi
Journal:  Toxicol Res       Date:  2018-10-15
  6 in total

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