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In vitro evaluation of the selective cytotoxicity and genotoxicity of three synthetic ortho-nitrobenzyl derivatives in human cancer cell lines, with and without metabolic activation

遗传毒性 细胞毒性 克隆形成试验 化学 微核试验 彗星试验 微核 MTT法 癌细胞 致癌物 生物化学 活力测定 雷苏林 DNA损伤 体外 体外毒理学 细胞培养 药理学 生物 癌症 毒性 DNA 遗传学 有机化学
作者
Júlia Teixeira de Oliveira,Kimberly Brito Tecchio,Marcela Silva Lopes,Silmara Nunes Andrade,Rosy Iara Maciel de Azambuja Ribeiro,Fernando de Pilla Varotti,Renata Barbosa de Oliveira,Gustavo Henrique Ribeiro Viana,Vanessa Jaqueline da Silva Vieira dos Santos,Fábio Vieira dos Santos
出处
期刊:Drug and Chemical Toxicology [Informa]
卷期号:47 (4): 404-415
标识
DOI:10.1080/01480545.2023.2184478
摘要

Although the presence of nitro groups in chemicals can be recognized as structural alerts for mutagenicity and carcinogenicity, nitroaromatic compounds have attracted considerable interest as a class of agents that can serve as source of potential new anticancer agents. In the present study, the in vitro cytotoxicity, genotoxicity, and mutagenicity of three synthetic ortho-nitrobenzyl derivatives (named ON-1, ON-2 and ON-3) were evaluated by employing human breast and ovarian cancer cell lines. A series of biological assays was carried out with and without metabolic activation. Complementarily, computational predictions of the pharmacokinetic properties and druglikeness of the compounds were performed in the Swiss ADME platform. The MTT assay showed that the compounds selectively affected selectively the cell viability of cancer cells in comparison with a nontumoral cell line. Additionally, the metabolic activation enhanced cytotoxicity, and the compounds affected cell survival, as demonstrated by the clonogenic assay. The comet assay, the cytokinesis-block micronucleus assay, and the immunofluorescence of the γ-H2AX foci formation assay have that the compounds caused chromosomal damage to the cancer cells, with and without metabolic activation. The results obtained in the present study showed that the compounds assessed were genotoxic and mutagenic, inducing double-strand breaks in the DNA structure. The high selectivity indices observed for the compounds ON-2 and ON-3, especially after metabolic activation with the S9 fraction, must be highlighted. These experimental biological results, as well as the theoretical properties predicted for the compounds have shown that they are promising anticancer candidates to be exploited in additional studies.
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