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CRISPR-Cas9 cytidine and adenosine base editing of splice-sites mediates highly-efficient disruption of proteins in primary and immortalized cells

Author

Listed:
  • Mitchell G. Kluesner

    (University of Minnesota
    University of Minnesota
    University of Minnesota
    University of Minnesota)

  • Walker S. Lahr

    (University of Minnesota
    University of Minnesota
    University of Minnesota
    University of Minnesota)

  • Cara-lin Lonetree

    (University of Minnesota
    University of Minnesota
    University of Minnesota
    University of Minnesota)

  • Branden A. Smeester

    (University of Minnesota
    University of Minnesota
    University of Minnesota
    University of Minnesota)

  • Xiaohong Qiu

    (University of Minnesota
    University of Minnesota
    University of Minnesota
    University of Minnesota)

  • Nicholas J. Slipek

    (University of Minnesota
    University of Minnesota
    University of Minnesota
    University of Minnesota)

  • Patricia N. Claudio Vázquez

    (University of Minnesota
    University of Minnesota
    University of Minnesota
    University of Minnesota)

  • Samuel P. Pitzen

    (University of Minnesota
    University of Minnesota)

  • Emily J. Pomeroy

    (University of Minnesota
    University of Minnesota
    University of Minnesota
    University of Minnesota)

  • Madison J. Vignes

    (University of Minnesota)

  • Samantha C. Lee

    (University of Minnesota
    University of Minnesota)

  • Samuel P. Bingea

    (University of Minnesota
    University of Minnesota
    University of Minnesota
    University of Minnesota)

  • Aneesha A. Andrew

    (University of Minnesota
    University of Minnesota)

  • Beau R. Webber

    (University of Minnesota
    University of Minnesota
    University of Minnesota
    University of Minnesota)

  • Branden S. Moriarity

    (University of Minnesota
    University of Minnesota
    University of Minnesota
    University of Minnesota)

Abstract

CRISPR-Cas9 cytidine and adenosine base editors (CBEs and ABEs) can disrupt genes without introducing double-stranded breaks by inactivating splice sites (BE-splice) or by introducing premature stop (pmSTOP) codons. However, no in-depth comparison of these methods or a modular tool for designing BE-splice sgRNAs exists. To address these needs, we develop SpliceR ( http://z.umn.edu/spliceR ) to design and rank BE-splice sgRNAs for any Ensembl annotated genome, and compared disruption approaches in T cells using a screen against the TCR-CD3 MHC Class I immune synapse. Among the targeted genes, we find that targeting splice-donors is the most reliable disruption method, followed by targeting splice-acceptors, and introducing pmSTOPs. Further, the CBE BE4 is more effective for disruption than the ABE ABE7.10, however this disparity is eliminated by employing ABE8e. Collectively, we demonstrate a robust method for gene disruption, accompanied by a modular design tool that is of use to basic and translational researchers alike.

Suggested Citation

  • Mitchell G. Kluesner & Walker S. Lahr & Cara-lin Lonetree & Branden A. Smeester & Xiaohong Qiu & Nicholas J. Slipek & Patricia N. Claudio Vázquez & Samuel P. Pitzen & Emily J. Pomeroy & Madison J. Vig, 2021. "CRISPR-Cas9 cytidine and adenosine base editing of splice-sites mediates highly-efficient disruption of proteins in primary and immortalized cells," Nature Communications, Nature, vol. 12(1), pages 1-12, December.
  • Handle: RePEc:nat:natcom:v:12:y:2021:i:1:d:10.1038_s41467-021-22009-2
    DOI: 10.1038/s41467-021-22009-2
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    Cited by:

    1. Hongzhi Zeng & Qichen Yuan & Fei Peng & Dacheng Ma & Ananya Lingineni & Kelly Chee & Peretz Gilberd & Emmanuel C. Osikpa & Zheng Sun & Xue Gao, 2023. "A split and inducible adenine base editor for precise in vivo base editing," Nature Communications, Nature, vol. 14(1), pages 1-14, December.

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