3,5-Dimethyaminophenol is not Mutagenic in Ames Test and HPRT Test and may have Anti-Carcinogenic Potential Against Lung Cancer Cells

Ming-Wei Chao; Chia-Yi Tseng; Pei-Ying Lin; Yu-Jung Chang; Özge Köse; Suna Sabuncuoğlu; Yu-Chen Chen; Chin-Hung Lin; Belma Kocer-Gumusel; Pınar Erkekoglu

doi:10.3390/proceedings2251553

Proceedings (Dec 2018)

3,5-Dimethyaminophenol is not Mutagenic in Ames Test and HPRT Test and may have Anti-Carcinogenic Potential Against Lung Cancer Cells

Ming-Wei Chao,
Chia-Yi Tseng,
Pei-Ying Lin,
Yu-Jung Chang,
Özge Köse,
Suna Sabuncuoğlu,
Yu-Chen Chen,
Chin-Hung Lin,
Belma Kocer-Gumusel,
Pınar Erkekoglu

Affiliations

Ming-Wei Chao: Center of Biomedicine, College of Engineering, Chung Yuan Christian University, Zhongli District, Taoyuan 320, Taiwan
Chia-Yi Tseng: Department of Biomedical Engineering, Chung Yuan Christian University, Zhongli District, Taoyuan 320, Taiwan
Pei-Ying Lin: Department of Bioscience Technology, Chung Yuan Christian University, Zhongli District, Taoyuan 320, Taiwan
Yu-Jung Chang: Department of Bioscience Technology, Chung Yuan Christian University, Zhongli District, Taoyuan 320, Taiwan
Özge Köse: Hacettepe University, Faculty of Pharmacy, Department of Toxicology, Sıhhiye, 06100 Ankara, Turkey
Suna Sabuncuoğlu: Hacettepe University, Faculty of Pharmacy, Department of Toxicology, Sıhhiye, 06100 Ankara, Turkey
Yu-Chen Chen: Department of Radiology, Taoyuan General Hospital, Taoyuan district, Taoyuan 320, Taiwan
Chin-Hung Lin: Department of Bioscience Technology, Chung Yuan Christian University, Zhongli District, Taoyuan 320, Taiwan
Belma Kocer-Gumusel: Lokman Hekim University, Faculty of Pharmacy, Department of Toxicology, 06100 Ankara, Turkey
Pınar Erkekoglu: Hacettepe University, Faculty of Pharmacy, Department of Toxicology, Sıhhiye, 06100 Ankara, Turkey

DOI: https://doi.org/10.3390/proceedings2251553
Journal volume & issue: Vol. 2, no. 25
p. 1553

Abstract

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Exposure to 3,5-dimethylaminophenol (3,5-DMAP), the metabolite of the 3-5-dimethylaniline, was shown to cause high levels of oxidative stress in different cells. However, we have shown that this alkylaniline metabolite was non-mutagenic to different strains of Salmonella typhimurium in Ames test and also was found to be not mutagenic to CHO cells in HPRT test. Concerning all the available data, we aimed to observe whether this metabolite may have anti-carcinogenic potential in human non-small cell lung cancer line (A549 cells). 3,5-DMAP caused a dose-dependent increase in cytotoxicity and generation of superoxide (O2-.) and reactive oxygen species (ROS). 3,5-DMAP did not produce significant cytotoxicity to human lung fibroblasts even at very high concentrations; however showed higher cytotoxic effect on A549 lung cancer cells at the same concentrations. 3,5-DMAP also led to molecular events, like increases in apoptotic markers (i.e., p53, Bad, Bax and cytochrome and decreases anti-apoptotic proteins (Bcl-2). Furthermore, 3,5-DMAP provided significant decreases in cell viability of A549 cells and eventually inhibited growth of A549 cells in an in vivo mouse model. Tumor sections showed that 3,5-DMAP down-regulated c-Myc expression but up-regulated p53 and cytochrome c, all of which might result in tumor growth arrest. In conclusion, our findings demonstrate 3,5-DMAP is not mutagenic to Salmonella typhimurium and CHO cells; toxic to A549 cells and therefore may have anti-cancer properties, the importance of which should be elucidated with further mechanistic studies.

Published in Proceedings

ISSN: 2504-3900 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: General Works
Website: http://www.mdpi.com/journal/proceedings

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