Communications Biology (Mar 2025)

SunTag-PE: a modular prime editing system enables versatile and efficient genome editing

  • Jiashuo Liu,
  • Jingjing Zhang,
  • Tingting Zhao,
  • Mengya Zhao,
  • Min Su,
  • Ye Chen,
  • Zheying Huang,
  • Yuyan Wang,
  • Chaoyue Zhong,
  • Zheng Hu,
  • Ping Zhou,
  • Rui Tian,
  • Dan He

DOI
https://doi.org/10.1038/s42003-025-07893-4
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 9

Abstract

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Abstract Prime editing (PE) holds tremendous potential in the treatment of genetic diseases because it can install any desired base substitution or local insertion/deletion. However, the full-length PE effector size (6.3-kb) is beyond the packaging capacity of adeno-associated virus (AAV), hindering its clinical translation. Various splitting strategies have been used to improve its delivery, but always accompanied by compromised PE efficiency. Here, we developed a modular and efficient SunTag-PE system that splits PE effectors into GCN4-nCas9 and single-chain variable fragment (scFv) tethered reverse transcriptase (RT). We observed that SunTag-PEs with 1×GCN4 in the N terminus of nCas9 was the most efficient configuration rather than multiple copies of GCN4. This SunTag-PE strategy achieved editing levels comparable to canonical fused-PE (nCas9 and RT are linked together) and higher than other split-PE strategies (including sPE and MS2-PE) in both PE2 and PE3 forms with no increase in insertion and deletion (indel) byproducts. Moreover, we successfully validated the modularity of SunTag-PE system in the Cas9 orthologs of SauCas9 and FrCas9. Finally, we employed dual AAVs to deliver SunTag-ePE3 and efficiently corrected the pathogenic mutation in HBB mutant cell line. Collectively, our SunTag-PE system provides an efficient modular splitting strategy for prime editing and further facilitate its transformation in clinics.