Molecular Therapy: Nucleic Acids (Jun 2022)

Engineering of near-PAMless adenine base editor with enhanced editing activity and reduced off-target

  • Xiaofang Cao,
  • Junfan Guo,
  • Shisheng Huang,
  • Wenxia Yu,
  • Guanglei Li,
  • Lisha An,
  • Xiangyang Li,
  • Wanyu Tao,
  • Qing Liu,
  • Xingxu Huang,
  • Xiaohua Jin,
  • Xu Ma

Journal volume & issue
Vol. 28
pp. 732 – 742

Abstract

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About 47% of pathogenic point mutations could be corrected by ABE-induced A·T-to-G·C conversions. However, the applications of ABEs are still hindered by undesired editing efficiency, limited editing scopes, and off-targeting effects. Here, we develop a new adenine base editor, by embedding TadA-8e monomer into SpRY-nCas9, named as CE-8e-SpRY, which exhibits higher activity at NRN than NYN PAMs favored by SpRY nuclease. CE-8e-SpRY could target nearly all genomic sites in principle and induces the highest targeting efficiency among tested SpRY-based ABEs. In addition, CE-8e-SpRY also shows reduced RNA and DNA off-targeting activities. With optimized sgRNAs, CE-8e-SpRY induces efficient or desired target editing at some disease-relevant loci where conventional ABEs were unable to induce precise and satisfied editing. Taken together, our CE-8e-SpRY could broaden the applicability of ABEs in correcting or introducing pathogenic point mutations.

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