A dual-deaminase CRISPR base editor enables concurrent adenine and cytosine editing.
Julian GrünewaldRonghao ZhouCaleb A LareauSara P GarciaSowmya IyerBret R MillerLukas M LangnerJonathan Y HsuMartin J AryeeJ Keith JoungPublished in: Nature biotechnology (2020)
Existing adenine and cytosine base editors induce only a single type of modification, limiting the range of DNA alterations that can be created. Here we describe a CRISPR-Cas9-based synchronous programmable adenine and cytosine editor (SPACE) that can concurrently introduce A-to-G and C-to-T substitutions with minimal RNA off-target edits. SPACE expands the range of possible DNA sequence alterations, broadening the research applications of CRISPR base editors.