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The Carcinogenic Potential of Bisphenol A in the Liver Based on Transcriptomic Studies

CANCERS(2023)

Cited 1|Views32
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Abstract
Simple Summary Bisphenol A (BPA), an endocrine-disrupting chemical extensively used in the production of everyday products, profoundly affects human homeostasis and well-being. Given the liver's critical role in toxins' first passage detoxification, it may become highly susceptible to BPA harmful effects. The present study aimed at investigating changes in the liver transcriptomics caused by oral exposure to BPA in mice. Our findings may contribute to clarifying the impact of BPA on gene expression in mice livers to predict the molecular mechanisms underlying BPA-related hepatic toxicity and carcinogenic effect.Abstract Bisphenol A (BPA) is an environmental toxin widely used in the production of polycarbonate plastics. A correlation exists between BPA tissue contamination and the occurrence of pathological conditions, including cancer. First-passage detoxification of high BPA amounts in the liver promotes hepatotoxicity and morphological alterations of this organ, but there is a lack of knowledge about the molecular mechanisms underlying these phenomena. This prompted us to investigate changes in the liver transcriptomics of 3-month-old female mice exposed to BPA (50 mg/kg) in drinking water for 3 months. Five female mice served as controls. The animals were euthanized, the livers were collected, and RNA was extracted to perform RNA-seq analysis. The multistep transcriptomic bioinformatics revealed 120 differentially expressed genes (DEGs) in the BPA-exposed samples. Gene Ontology (GO) annotations indicated that DEGs have been assigned to many biological processes, including "macromolecule modification" and "protein metabolic process". Several of the revealed DEGs have been linked to the pathogenesis of severe metabolic liver disorders and malignant tumors, in particular hepatocellular carcinoma. Data from this study suggest that BPA has a significant impact on gene expression in the liver, which is predictive of the carcinogenic potential of this compound in this organ.
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Key words
bisphenol A,liver,mitochondrial dysfunction,hepatocellular carcinoma,RNA-Seq
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