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Incorporation of Pseudouridine Into mRNA Yields Superior Nonimmunogenic Vector With Increased Translational Capacity and Biological Stability

机译:将假性尿苷掺入mRNA产生具有提高的翻译能力和生物稳定性的优良的非免疫原性载体

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摘要

In vitro–transcribed mRNAs encoding physiologically important proteins have considerable potential for therapeutic applications. However, in its present form, mRNA is unfeasible for clinical use because of its labile and immunogenic nature. Here, we investigated whether incorporation of naturally modified nucleotides into transcripts would confer enhanced biological properties to mRNA. We found that mRNAs containing pseudouridines have a higher translational capacity than unmodified mRNAs when tested in mammalian cells and lysates or administered intravenously into mice at 0.015–0.15 mg/kg doses. The delivered mRNA and the encoded protein could be detected in the spleen at 1, 4, and 24 hours after the injection, where both products were at significantly higher levels when pseudouridine-containing mRNA was administered. Even at higher doses, only the unmodified mRNA was immunogenic, inducing high serum levels of interferon-α (IFN-α). These findings indicate that nucleoside modification is an effective approach to enhance stability and translational capacity of mRNA while diminishing its immunogenicity in vivo. Improved properties conferred by pseudouridine make such mRNA a promising tool for both gene replacement and vaccination.
机译:体外转录的编码具有重要生理意义的蛋白质的mRNA具有巨大的治疗应用潜力。然而,由于其不稳定和免疫原性,以目前的形式,mRNA在临床上是不可行的。在这里,我们调查了将天然修饰的核苷酸掺入转录本是否会赋予mRNA增强的生物学特性。我们发现,在哺乳动物细胞和裂解物中或以0.015-0.15 mg / kg剂量静脉内施用给小鼠时,含有假尿苷的mRNA的翻译能力要高于未修饰的mRNA。注射后1、4和24小时,可以在脾脏中检测到递送的mRNA和编码的蛋白质,当使用含假尿苷的mRNA时,两种产品的含量均显着较高。即使在较高剂量下,也只有未修饰的mRNA具有免疫原性,从而导致高血清干扰素-α(IFN-α)水平。这些发现表明,核苷修饰是增强mRNA的稳定性和翻译能力同时降低其体内免疫原性的有效方法。伪尿苷赋予的改进的性质使这种mRNA成为用于基因替换和疫苗接种的有前途的工具。

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