Evaluation of the effects of polybrominated diphenyl ethers congeners, BDE-100 and BDE-153, on the HepG2 cell line

The brominated flame retardants are substances used in consumer goods to increase its fire resistance and/or high temperatures. Due to, the polybrominated diphenyl ethers (Polybrominated diphenyl ether) are the most commonly used class in view of its efficiency in controlling the spread of flame and low cost. These compounds are considered persistent, bioaccumulative, can be transported over long distances and have toxicity. However the toxic mechanisms of action have not been well established. Thus, this project held cytotoxic, genotoxic and mutagenic assays in HepG2, HeLa, hepatocytes and human lymphocytes cells in order to elucidate the mechanisms of toxicity. The results demonstrate the ability of these compounds to induce primary DNA damage (0.5 ?M for BDE-153 and 5 ?M for BDE-100) monitored by the comet assay, it was not repaired after 24 hours of exposure. However, there was not observed nether increase in micronuclei in HepG2 cells and lymphocytes after exposure to the congeners (0.1 - 25 ?M) even in the Salmonella typhimurium mutagenicity assay. However, the compounds show the ability to reduce MTT reduction, proliferation, and interfere with cell cycle evaluated in cell cultures. These cytotoxic effects are related to mitochondrial dysfunction, since both PBDE generate dissipation of the mitochondrial membrane potential, accumulation of reactive oxygen species, resulting in apoptotic cell death, demonstrated by the maintenance of serine phosphatidyl on the external surface of the cell membrane, by condensation and nuclear fragmentation, the presence of pro-apoptotic factors in the cytosol of the cell, such as cytochrome c and AIF plus activating caspase 3 and 9. These data corroborate the fact of not having to intracellular lactate dehydrogenase release, excluding death cell necrosis. Finally, it was observed that exposure to the active compounds the autophagic process, at first as a cytoprotective mechanism observed by LC3I conversion in LC3II and accumulation of p62 (autophagic markers) plus imunicitoquímicas markings for LC3II and co-location lysosomes in dotted pattern, indicanto accumulations of LC3 protein and lysosomes, forming autophagosomes. Together our results show the ability to induce genomic instability and cytotoxicity of this class of compounds, reinforcing the idea that PBDEs pose a risk to the exposed population (AU)