作者
Alexandra G Orlandini von Niessen, Marco A Poleganov, Corina Rechner, Arianne Plaschke, Lena M Kranz, Stephanie Fesser, Mustafa Diken, Martin Löwer, Britta Vallazza, Tim Beissert, Valesca Bukur, Andreas N Kuhn, Özlem Türeci, Ugur Sahin
发表日期
2019/4/10
期刊
Molecular Therapy
卷号
27
期号
4
页码范围
824-836
出版商
Elsevier
简介
Synthetic mRNA has emerged as a powerful tool for the transfer of genetic information, and it is being explored for a variety of therapeutic applications. Many of these applications require prolonged intracellular persistence of mRNA to improve bioavailability of the encoded protein. mRNA molecules are intrinsically unstable and their intracellular kinetics depend on the UTRs embracing the coding sequence, in particular the 3′ UTR elements. We describe here a novel and generally applicable cell-based selection process for the identification of 3′ UTRs that augment the expression of proteins encoded by synthetic mRNA. Moreover, we show, for two applications of mRNA therapeutics, namely, (1) the delivery of vaccine antigens in order to mount T cell immune responses and (2) the introduction of reprogramming factors into differentiated cells in order to induce pluripotency, that mRNAs tagged with the 3′ UTR …
引用总数
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