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Enhancement of prime editing via xrRNA motif-joined pegRNA.


ABSTRACT: The prime editors (PEs) have shown great promise for precise genome modification. However, their suboptimal efficiencies present a significant technical challenge. Here, by appending a viral exoribonuclease-resistant RNA motif (xrRNA) to the 3'-extended portion of pegRNAs for their increased resistance against degradation, we develop an upgraded PE platform (xrPE) with substantially enhanced editing efficiencies in multiple cell lines. A pan-target average enhancement of up to 3.1-, 4.5- and 2.5-fold in given cell types is observed for base conversions, small deletions, and small insertions, respectively. Additionally, xrPE exhibits comparable edit:indel ratios and similarly minimal off-target editing as the canonical PE3. Of note, parallel comparison of xrPE to the most recently developed epegRNA-based PE system shows their largely equivalent editing performances. Our study establishes a highly adaptable platform of improved PE that shall have broad implications.

SUBMITTER: Zhang G 

PROVIDER: S-EPMC8986804 | biostudies-literature | 2022 Apr

REPOSITORIES: biostudies-literature

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Enhancement of prime editing via xrRNA motif-joined pegRNA.

Zhang Guiquan G   Liu Yao Y   Huang Shisheng S   Qu Shiyuan S   Cheng Daolin D   Yao Yuan Y   Ji Quanjiang Q   Wang Xiaolong X   Huang Xingxu X   Liu Jianghuai J  

Nature communications 20220406 1


The prime editors (PEs) have shown great promise for precise genome modification. However, their suboptimal efficiencies present a significant technical challenge. Here, by appending a viral exoribonuclease-resistant RNA motif (xrRNA) to the 3'-extended portion of pegRNAs for their increased resistance against degradation, we develop an upgraded PE platform (xrPE) with substantially enhanced editing efficiencies in multiple cell lines. A pan-target average enhancement of up to 3.1-, 4.5- and 2.5  ...[more]

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