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首页> 外文期刊>Nucleic Acids Research >N-1-Methylpseudouridine substitution enhances the performance of synthetic mRNA switches in cells
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N-1-Methylpseudouridine substitution enhances the performance of synthetic mRNA switches in cells

机译:N-1-甲基哌嗪取代增强了细胞中合成mRNA开关的性能

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摘要

Synthetic messenger RNA (mRNA) tools often use pseudouridine and 5-methyl cytidine as substitutions for uridine and cytidine to avoid the immune response and cytotoxicity induced by introducing mRNA into cells. However, the influence of base modifications on the functionality of the RNA tools is poorly understood. Here we show that synthetic mRNA switches containing N(1-)Methylpseudouridine (m1 Psi) as a substitution of uridine substantially out-performed all other modified bases studied, exhibiting enhanced microRNA and protein sensitivity, better cell-type separation ability, and comparably low immune stimulation. We found that the observed phenomena stern from the high protein expression from ml containing mRNA and efficient translational repression in the presence of target microRNAs or proteins. In addition, synthetic gene circuits with m1 Psi significantly improve performance in cells. These findings indicate that synthetic mRNAs with m1 Psi modification have enormous potentials in the research and application of biofunctional RNA tools.
机译:合成信使RNA(mRNA)工具通常使用假尿素和5-甲基胞嘧啶作为尿苷和胞苷的取代,以避免通过将mRNA引入细胞中的免疫应答和细胞毒性。然而,基础修改对RNA工具功能的影响很差。在这里,我们表明,含有N(1-)甲基己酰胺(M1 PSI)的合成mRNA开关作为尿苷的取代,基本上除了研究的所有其他修饰的碱基,表现出增强的MicroRNA和蛋白质敏感性,更好的细胞型分离能力,并且相当低免疫刺激。我们发现观察到的现象从含有mRNA的M1的高蛋白质表达中苛刻,并且在靶微型瘤或蛋白质存在下的有效平移抑制。此外,具有M1 PSI的合成基因电路显着提高细胞中的性能。这些发现表明,具有M1 PSI修改的合成MRNA具有生物功能RNA工具的研究和应用具有巨大潜力。

著录项

  • 来源
    《Nucleic Acids Research》 |2020年第6期|共9页
  • 作者单位

    Kyoto Univ Ctr iPS Cell Res &

    Applicat Dept Life Sci Frontiers Sakyo Ku 53 Kawaharacho Kyoto 6068507 Japan;

    Kyoto Univ Ctr iPS Cell Res &

    Applicat Dept Life Sci Frontiers Sakyo Ku 53 Kawaharacho Kyoto 6068507 Japan;

    Kyoto Univ Ctr iPS Cell Res &

    Applicat Dept Life Sci Frontiers Sakyo Ku 53 Kawaharacho Kyoto 6068507 Japan;

    Kyoto Univ Ctr iPS Cell Res &

    Applicat Dept Life Sci Frontiers Sakyo Ku 53 Kawaharacho Kyoto 6068507 Japan;

    Kyoto Univ Ctr iPS Cell Res &

    Applicat Dept Life Sci Frontiers Sakyo Ku 53 Kawaharacho Kyoto 6068507 Japan;

    Kyoto Univ Grad Sch Sci Dept Chem Sakyo Ku Kyoto 6068502 Japan;

    Kyoto Univ Grad Sch Sci Dept Chem Sakyo Ku Kyoto 6068502 Japan;

    Kyoto Univ Grad Sch Sci Dept Chem Sakyo Ku Kyoto 6068502 Japan;

    Hong Kong Univ Sci &

    Technol Dept Chem &

    Biol Engn Kowloon Room 5578 Acad Bldg Clear Water Bay Hong Kong Peoples R China;

    Kyoto Univ Ctr iPS Cell Res &

    Applicat Dept Life Sci Frontiers Sakyo Ku 53 Kawaharacho Kyoto 6068507 Japan;

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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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