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Engineering TALE-linked deaminases to facilitate precision adenine base editing in mitochondrial DNA

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Authors

Cho, Sung-Ik; Lim, Kayeong; Hong, Seongho; Lee, Jaesuk; Kim, Annie; Lim, Chae Jin; Ryou, Seungmin; Lee, Ji Min; Mok, Young Geun; Chung, Eugene; Kim, Sanghun; Han, Seunghun; Cho, Sang-Mi; Kim, Jieun; Kim, Eun-Kyoung; Nam, Ki-Hoan; Oh, Yeji; Choi, Minkyung; An, Tae Hyeon; Oh, Kyoung-Jin; Lee, Seonghyun; Lee, Hyunji; Kim, Jin-Soo

Issue Date
2024-01
Publisher
Elsevier B.V.
Citation
Cell, Vol.187 No.1, pp.95-109.e26
Abstract
DddA-derived cytosine base editors (DdCBEs) and transcription activator-like effector (TALE)-linked deaminases (TALEDs) catalyze targeted base editing of mitochondrial DNA (mtDNA) in eukaryotic cells, a method useful for modeling of mitochondrial genetic disorders and developing novel therapeutic modalities. Here, we report that A-to-G-editing TALEDs but not C-to-T-editing DdCBEs induce tens of thousands of transcriptome-wide off-target edits in human cells. To avoid these unwanted RNA edits, we engineered the substrate-binding site in TadA8e, the deoxy-adenine deaminase in TALEDs, and created TALED variants with fine-tuned deaminase activity. Our engineered TALED variants not only reduced RNA off-target edits by >99% but also minimized off-target mtDNA mutations and bystander edits at a target site. Unlike wild-type versions, our TALED variants were not cytotoxic and did not cause developmental arrest of mouse embryos. As a result, we obtained mice with pathogenic mtDNA mutations, associated with Leigh syndrome, which showed reduced heart rates.
ISSN
0092-8674
URI
https://hdl.handle.net/10371/198907
DOI
https://doi.org/10.1016/j.cell.2023.11.035
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  • College of Natural Sciences
  • Department of Chemistry
Research Area Biology and Biochemistry

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