寡核苷酸
核糖核酸
寡核苷酸合成
组合化学
化学
酶
核苷酸
计算生物学
生物化学
生物
DNA
基因
作者
Daniel J. Wiegand,Jonathan Rittichier,Ella Meyer,Howon Lee,Nicholas J. Conway,Daniel Ahlstedt,Zeynep Yurtsever,Dominic Rainone,Erkin Kuru,George M. Church
标识
DOI:10.1038/s41587-024-02244-w
摘要
Abstract RNA oligonucleotides have emerged as a powerful therapeutic modality to treat disease, yet current manufacturing methods may not be able to deliver on anticipated future demand. Here, we report the development and optimization of an aqueous-based, template-independent enzymatic RNA oligonucleotide synthesis platform as an alternative to traditional chemical methods. The enzymatic synthesis of RNA oligonucleotides is made possible by controlled incorporation of reversible terminator nucleotides with a common 3′- O -allyl ether blocking group using new CID1 poly(U) polymerase mutant variants. We achieved an average coupling efficiency of 95% and demonstrated ten full cycles of liquid phase synthesis to produce natural and therapeutically relevant modified sequences. We then qualitatively assessed the platform on a solid phase, performing enzymatic synthesis of several N + 5 oligonucleotides on a controlled-pore glass support. Adoption of an aqueous-based process will offer key advantages including the reduction of solvent use and sustainable therapeutic oligonucleotide manufacturing.
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