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Epigenetic modification of cytosines fine tunes the stability of i-motif DNA

机译:细胞瘤的表观遗传改性细小曲调I-MOTIF DNA的稳定性

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摘要

i-Motifs are widely used in nanotechnology, play a part in gene regulation and have been detected in human nuclei. As these structures are composed of cytosine, they are potential sites for epigenetic modification. In addition to 5-methyl- and 5-hydroxymethylcytosine modifications, recent evidence has suggested biological roles for 5-formylcytosine and 5-carboxylcytosine. Herein the human telomeric i-motif sequence was used to examine how these four epigenetic modifications alter the thermal and pH stability of i-motifs. Changes in melting temperature and transitional pH depended on both the type of modification and its position within the i-motif forming sequence. The cytosines most sensitive to modification were next to the first and third loops within the structure. Using previously described i-motif forming sequences, we screened the MCF-7 and MCF-10A methylomes to map 5-methylcytosine and found the majority of sequences were differentially methylated in MCF7 (cancerous) and MCF10A (non-cancerous) cell lines. Furthermore, i-motif forming sequences stable at neutral pH were significantly more likely to be epigenetically modified than traditional acidic i-motif forming sequences. This work has implications not only in the epigenetic regulation of DNA, but also allows discreet tunability of i-motif stability for nanotechnological applications.
机译:I-MOTIF广泛用于纳米技术,在基因调节中发挥作用,并在人体核中进行了检测。由于这些结构由胞嘧啶组成,因此它们是表观遗传改性的潜在部位。除了5-甲基和5-羟甲基甲基胞嘧啶修饰外,最近的证据表明5-甲酰基胞嘧啶和5-羧胞苷的生物学作用。在此用于检查这四种表观遗传修饰如何改变I-MOTIF的热量和pH稳定性的方法。熔融温度和过渡性pH的变化依赖于I-MOTIF形成序列内的修饰类型及其位置。对修饰最敏感的胞嘧啶旁边是结构内的第一和第三环。使用先前描述的I-MOTIF形成序列,我们筛选MCF-7和MCF-10A甲基胚源来映射5-甲基胞嘧啶,发现大部分序列在MCF7(癌症)和MCF10A(非癌症)细胞系中差异甲基化。此外,在中性pH下稳定的I-MOTIF形成序列比传统的酸性I-MOTIF形成序列显着更容易被外观改性。这项工作不仅在DNA的表观遗传调节中产生了影响,而且还允许对纳米技术应用的I-MOTIF稳定性进行谨慎的可调性。

著录项

  • 来源
    《Nucleic Acids Research》 |2020年第1期|共8页
  • 作者单位

    Univ East Anglia Sch Pharm Norwich Res Pk Norwich NR4 7TJ Norfolk England;

    Univ East Anglia Sch Pharm Norwich Res Pk Norwich NR4 7TJ Norfolk England;

    Univ East Anglia Sch Pharm Norwich Res Pk Norwich NR4 7TJ Norfolk England;

    Univ Western Australia Sch Mol Sci 35 Stirling Hwy Crawley WA 6009 Australia;

    Univ Western Australia Sch Mol Sci 35 Stirling Hwy Crawley WA 6009 Australia;

    Univ Western Australia Sch Mol Sci 35 Stirling Hwy Crawley WA 6009 Australia;

    Univ East Anglia Sch Pharm Norwich Res Pk Norwich NR4 7TJ Norfolk England;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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