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2. Adenine transversion editors enable precise, efficient A•T-to-C•G base editing in mammalian cells and embryos.

3. A prime editor mouse to model a broad spectrum of somatic mutations in vivo.

4. Efficient prime editing in mouse brain, liver and heart with dual AAVs.

5. Phage-assisted evolution and protein engineering yield compact, efficient prime editors.

6. Designing and executing prime editing experiments in mammalian cells.

8. Engineered pegRNAs improve prime editing efficiency.

9. Engineered virus-like particles for efficient in vivo delivery of therapeutic proteins.

10. Continuous evolution of SpCas9 variants compatible with non-G PAMs.

11. Search-and-replace genome editing without double-strand breaks or donor DNA.

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