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Sodium arsenite modulates histone acetylation, histone deacetylase activity and HMGN protein dynamics in human cells

机译:亚砷酸钠调节人细胞中的组蛋白乙酰化,组蛋白脱乙酰酶活性和HMGN蛋白动力学

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Extensive epidemiological data indicate that inorganic arsenic is associated with several types of human cancer. Nevertheless, the underlying mechanisms are poorly understood. Among its mode of action are the alterations on DNA methylation, which provoke aberrant gene expression. However, beyond DNA methylation, little is known about arsenic’s effects on chromatin. In this study, we investigated the effects of sodium arsenite (NaAsO2) on global histone modifications and nucleosome-associated proteins. Our findings revealed that NaAsO2 exposure significantly increases global histone acetylation. This effect was related to the inhibition of histone deacetylase (HDAC) activity because NaAsO2 was able to inhibit HDACs comparable to the well-known HDAC inhibitor trichostatin A (TSA). Furthermore, analyses of the dynamic properties of the nucleosome-associated high mobility group N proteins demonstrate that NaAsO2 elevates their mobility. Thus, our data suggest that NaAsO2 induces chromatin opening by histone hyperacetylation due to HDAC inhibition and increase of the mobility of nucleosome-associated proteins. As the chromatin compaction is crucial for the regulation of gene expression as well as for genome stability, we propose that chromatin opening by NaAsO2 may play a significant role to impart its genotoxic effects.
机译:大量的流行病学数据表明,无机砷与几种类型的人类癌症有关。然而,对潜在的机制了解甚少。其作用方式之一是引起甲基化异常的DNA甲基化改变。但是,除了DNA甲基化以外,砷对染色质的影响知之甚少。在这项研究中,我们研究了亚砷酸钠(NaAsO 2 )对整体组蛋白修饰和核小体相关蛋白的影响。我们的发现表明,NaAsO 2 的暴露显着增加了整体组蛋白的乙酰化。这种作用与组蛋白脱乙酰基酶(HDAC)活性的抑制有关,因为NaAsO 2 能够抑制HDAC,而HDAC与众所周知的HDAC抑制剂曲古抑菌素A(TSA)相当。此外,对核小体相关的高迁移率N族蛋白动力学特性的分析表明,NaAsO 2 提高了其迁移率。因此,我们的数据表明NaAsO 2 通过HDAC抑制和核小体相关蛋白的迁移性增加,通过组蛋白超乙酰化诱导染色质开放。由于染色质紧实对于调节基因表达以及基因组稳定性至关重要,因此我们认为NaAsO 2 开启染色质可能在赋予其遗传毒性作用中起重要作用。

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