首页> 外文期刊>Mutagenesis >DNA demethylation protects from cleavable complex stabilization and DNA strand breakage induced by the topoisomerase type I inhibitor camptothecin.
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DNA demethylation protects from cleavable complex stabilization and DNA strand breakage induced by the topoisomerase type I inhibitor camptothecin.

机译:DNA脱甲基保护免受I型拓扑异构酶抑制剂喜树碱诱导的可裂解复合物稳定和DNA链断裂。

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摘要

Methylation of cytosine in CpG sequences of the DNA in mammalian cells is an epigenetic feature regulated very exactly that bears importance for events like gene expression, DNA replication, transcription and genetic imprinting. Changes in the DNA methylation pattern, both hypermethylation and hypomethylation, have been observed in the carcinogenic process. These changes, in general, influence the DNA conformation in such a way that certain proteins are disturbed in their interactions with the molecule. In this paper, we investigated in cultured Chinese hamster ovary cells the influence of hypomethylation induced by the substitution of 5-aza-2'-deoxycytidine for cytidine in DNA on topoisomerase type I (topo I) function, measured as the capacity of the enzyme inhibitor camptothecin (CPT) to stabilize the topoisomerase-DNA complexes and to induce DNA strand breakage. Our results demonstrate that the degree of methylation in DNA correlates with the effectiveness of CPT to stabilize the topo I-DNA complexes and to induce DNA cleavage. A protective effect of hypomethylation, as a whole, has been observed.
机译:哺乳动物细胞中DNA的CpG序列中胞嘧啶的甲基化是一种非常精确地调控的表观遗传学特征,对诸如基因表达,DNA复制,转录和基因印迹等事件具有重要意义。在致癌过程中已观察到DNA甲基化模式的变化,包括高甲基化和低甲基化。这些变化通常以某种方式影响DNA构象的方式,使某些蛋白质与分子的相互作用受到干扰。在本文中,我们研究了在培养的中国仓鼠卵巢细胞中用5-氮杂-2'-脱氧胞苷替代DNA中的胞苷诱导的低甲基化对拓扑异构酶I型(拓扑I)功能的影响,以酶的能力来衡量喜树碱(CPT)抑制剂可稳定拓扑异构酶-DNA复合物并诱导DNA链断裂。我们的结果表明,DNA中的甲基化程度与CPT稳定拓扑I-DNA复合物并诱导DNA裂解的有效性相关。总体上已经观察到低甲基化的保护作用。

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