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Differential effect of estradiol and bisphenol A on Set8 and Sirt1 expression in prostate cancer

机译:雌二醇和双酚A对前列腺癌Set8和Sirt1表达的差异作用

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Exposure to estrogenic compounds has been shown to epigenetically reprogram the prostate and may contribute to prostate cancer. The goal of this study was to determine the effect of physiological doses of estradiol and bisphenol A (BPA) on the expression of histone modifying enzymes (HMEs) in prostate cancer. Using two human prostate cancer cell lines we examined the expression of Set8, a histone methyltransferase, and Sirt1, a histone deacetylase, after exposure to estrogen or BPA. These experiments were carried out in the presence of natural hormones to understand the impact of additional exposure to estrogen or BPA on HME expression. We found differential expression of the HMEs in the different models and between the different compounds. Further, we determined that the changes in gene expression occurred via estrogen receptor signaling using the ER antagonist, ICI 182,780 (fulvestrant). Interestingly we found that the combination of ICI with estrogen or BPA greatly affected the expression of Set8, even when the hormone alone had no effect. This study demonstrates that the effects of estrogen and BPA on HME expression vary and that the presence of both the estrogen receptor and androgen receptor may be important for therapeutic intervention.
机译:暴露于雌激素化合物已被证明能对前列腺进行表观遗传重编程,并可能导致前列腺癌。这项研究的目的是确定生理剂量的雌二醇和双酚A(BPA)对前列腺癌中组蛋白修饰酶(HMEs)表达的影响。使用两种人类前列腺癌细胞系,我们检测了暴露于雌激素或BPA后的组蛋白甲基转移酶Set8和组蛋白脱乙酰基酶Sirt1的表达。这些实验是在天然激素存在下进行的,以了解额外暴露于雌激素或BPA对HME表达的影响。我们发现HMEs在不同模型中以及不同化合物之间的差异表达。此外,我们确定使用ER拮抗剂ICI 182,780(fulvestrant)通过雌激素受体信号传导发生了基因表达的变化。有趣的是,我们发现ICI与雌激素或BPA的组合极大地影响了Set8的表达,即使仅激素也不起作用。这项研究表明雌激素和BPA对HME表达的影响各不相同,并且雌激素受体和雄激素受体的存在可能对治疗干预很重要。

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