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首页> 外文期刊>Scientific reports. >Long-term exposure to a ‘safe’ dose of bisphenol A reduced protein acetylation in adult rat testes
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Long-term exposure to a ‘safe’ dose of bisphenol A reduced protein acetylation in adult rat testes

机译:长期暴露于“安全”剂量的双酚A降低成年大鼠乙酰化的降低的蛋白质乙酰化

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Bisphenol A (BPA), a typical environmental endocrine-disrupting chemical, induces epigenetic inheritance. Whether histone acetylation plays a role in these effects of BPA is largely unknown. Here, we investigated histone acetylation in male rats after long-term exposure to a ‘safe’ dose of BPA. Twenty adult male rats received either BPA (50?μg/kg·bw/day) or a vehicle diet for 35 weeks. Decreased protein lysine-acetylation levels at approximately ~17?kDa and ~25?kDa, as well as decreased histone acetylation of H3K9, H3K27 and H4K12, were detected by Western blot analysis of testes from the treated rats compared with controls. Additionally, increased protein expression of deacetylase Sirt1 and reduced binding of Sirt1, together with increased binding of estrogen receptor β (ERβ) to caveolin-1 (Cav-1), a structural protein component of caveolar membranes, were detected in treated rats compared with controls. Moreover, decreased acetylation of Cav-1 was observed in the treated rats for the first time. Our study showed that long-term exposure to a ‘safe’ dose of BPA reduces histone acetylation in the male reproductive system, which may be related to the phenotypic paternal-to-offspring transmission observed in our previous study. The evidence also suggested that these epigenetic effects may be meditated by Sirt1 via competition with ERβ for binding to Cav-1.
机译:双酚A(BPA),典型的环境内分泌破坏化学品,诱导表观遗传遗传。组蛋白乙酰化在BPA对这些效果中起作用的作用在很大程度上是未知的。在这里,我们在长期暴露于“安全”的BPA后,在雄性大鼠中研究了组酮乙酰化。二十个成年雄性大鼠接受了BPA(50μg/ kg·bw / day)或车辆饮食35周。通过对对照的睾丸对照对照的检测,通过蛋白质赖氨酸 - KDA和〜25℃下减少蛋白质赖氨酸 - 乙酰化水平,以及H3K9,H3K27和H4K12的组酮乙酰化。另外,在处理的大鼠中,检测到脱乙酰酶SIRT1和SIRT1的结合和SIRT1的结合增加了Caveolar膜的结构蛋白组分的增加的蛋白质表达,以及Caveolar膜的结构蛋白组分。控制。此外,首次在处理过的大鼠中观察到CaV-1的乙酰化。我们的研究表明,长期暴露于“安全”剂量的BPA,减少了雄性生殖系统中的组蛋白乙酰化,这可能与我们之前的研究中观察到的表型父目到后代传输有关。证据还提出,这些表观遗传效应可以通过β通过与ERβ竞争的竞争来思考,用于与CAV-1结合。

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