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Liver and ovarian toxicities boosted by bisphenol and gamma radiation in female albino rats

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Bisphenol A (BPA), a carbon-based synthetic polymer compound, was newly classified as an environmental toxicant and an endocrine-disrupting chemical leading to abnormalities in cell proliferation, apoptosis, or migration that contributes to cancer development and progression. This study aims to evaluate the effect of the elevation of γ- radiation dose and BPA on the liver and ovaries of female rats. In this study, eighty female albino rats (130–150 g) were used in this work. Rats in this experiment received BPA in ethanol (50 mg/kg b. wt.) for 30 days, day after day, and in the irradiated groups, animals were administered BPA and then exposed to γ- radiation in doses (2, 4, and 6 Gy) one shot dose. Several members of the cytochrome family were examined. Exposure to γ-radiation and BPA showed an increase in cytochrome P450 and b5 fold change. Further, BPA and γ-radiation activate α and β estrogen receptors and also downregulate aromatase (CYT19) fold change. The current results also revealed that BPA and/or γ-radiation regulate the protein expression of the PI3K/Akt signaling pathway. The steroidogenic acute regulatory protein (StAR) appeared to be targeted by BPA and γ-radiation and its relative expression was elevated significantly by raising the γ-radiation dose. In conclusion, exposure to BPA, an endocrine-disrupting chemical, leads to marked toxicity. Additionally, toxicity is heightened by increasing the γ-radiation dose, either alone or in combination with BPA.
Title: Liver and ovarian toxicities boosted by bisphenol and gamma radiation in female albino rats
Description:
Bisphenol A (BPA), a carbon-based synthetic polymer compound, was newly classified as an environmental toxicant and an endocrine-disrupting chemical leading to abnormalities in cell proliferation, apoptosis, or migration that contributes to cancer development and progression.
This study aims to evaluate the effect of the elevation of γ- radiation dose and BPA on the liver and ovaries of female rats.
In this study, eighty female albino rats (130–150 g) were used in this work.
Rats in this experiment received BPA in ethanol (50 mg/kg b.
wt.
) for 30 days, day after day, and in the irradiated groups, animals were administered BPA and then exposed to γ- radiation in doses (2, 4, and 6 Gy) one shot dose.
Several members of the cytochrome family were examined.
Exposure to γ-radiation and BPA showed an increase in cytochrome P450 and b5 fold change.
Further, BPA and γ-radiation activate α and β estrogen receptors and also downregulate aromatase (CYT19) fold change.
The current results also revealed that BPA and/or γ-radiation regulate the protein expression of the PI3K/Akt signaling pathway.
The steroidogenic acute regulatory protein (StAR) appeared to be targeted by BPA and γ-radiation and its relative expression was elevated significantly by raising the γ-radiation dose.
In conclusion, exposure to BPA, an endocrine-disrupting chemical, leads to marked toxicity.
Additionally, toxicity is heightened by increasing the γ-radiation dose, either alone or in combination with BPA.

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