Nature Communications | Cheng Tianlin's Team Explores Novel Approaches in the Development of Base Editors, Screening Modified TadA Homologous Proteins to Achieve Simultaneous Editing of Cytosine and Adenine.-INSTITUTE FOR TRANSLATIONAL BRAIN RESEARCH

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Nature Communications | Cheng Tianlin's Team Explores Novel Approaches in the Development of Base Editors, Screening Modified TadA Homologous Proteins to Achieve Simultaneous Editing of Cytosine and Adenine.

Date:2023-01-29 ClickTimes:

Cytidine and adenosine deaminases are required for cytosine and adenine editing of base editors respectively, and no single deaminase could enable concurrent and comparable cytosine and adenine editing. Additionally, distinct properties of cytidine and adenosine deaminases lead to various types of off-target effects, including Cas9-indendepent DNA off-target effects for cytosine base editors (CBEs) and RNA off-target effects particularly severe for adenine base editors (ABEs). Here we demonstrate that 25 TadA orthologs could be engineered to generate functional ABEs, CBEs or ACBEs via single or double mutations, which display minimized Cas9-independent DNA off-target effects and genotoxicity, with orthologs B5ZCW4, Q57LE3, E8WVH3, Q13XZ4 and B3PCY2 as promising candidates for further engineering. Furthermore, RNA off-target effects of TadA ortholog-derived base editors could be further reduced or even eliminated by additional single mutation. Taken together, our work expands the base editing toolkits, and also provides important clues for the potential evolutionary process of deaminases.

paper link: https://doi.org/10.1038/s41467-023-36003-3

Prev:Nucleic Acids Research | Engineering of cytosine base editors with DNA damage minimization and editing scope diversification

Next:Nature Communications | Collaborating Researchers Cheng Tianlin, Qiu Zilong, and Zhao Xingming, Achieve TadA Reprogramming and the Development of a High-Precision Mini Base Editor.