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Engineering a precise adenine base editor with minimal bystander editing.
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Mitochondrial genome engineering coming-of-age.
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Targeted A-to-G base editing in human mitochondrial DNA with programmable deaminases.
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CRISPR-free base editors with enhanced activity and expanded targeting scope in mitochondrial and nuclear DNA.
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Comprehensive interrogation of the ADAR2 deaminase domain for engineering enhanced RNA editing activity and specificity.
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