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Adenine base editor engineering reduces editing of bystander cytosines

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Title
Adenine base editor engineering reduces editing of bystander cytosines
Author(s)
Jeong, You Kyeong; Lee, SeokHoon; Hwang, Gue-Ho; Hong, Sung-Ah; Park, Se-eun; Jin-Soo Kim; Woo, Jae-Sung; Bae, Sangsu
Publication Date
2021-11
Journal
NATURE BIOTECHNOLOGY, v.39, no.11, pp.1426 - 1433
Publisher
NATURE RESEARCH
Abstract
Adenine base editors (ABEs) catalyze specific A-to-G conversions at genomic sites of interest. However, ABEs also induce cytosine deamination at the target site. To reduce the cytosine editing activity, we engineered a commonly used adenosine deaminase, TadA7.10, and found that ABE7.10 with a D108Q mutation in TadA7.10 exhibited tenfold reduced cytosine deamination activity. The D108Q mutation also reduces cytosine deamination activity in two recently developed high-activity versions of ABE, ABE8e and ABE8s, and is compatible with V106W, a mutation that reduces off-target RNA editing. ABE7.10 containing a P48R mutation displayed increased cytosine deamination activity and a substantially reduced adenine editing rate, yielding a TC-specific base editing tool for TC-to-TT or TC-to-TG conversions that broadens the utility of base editors. Engineered variants of adenine base editors have reduced cytosine base editing or a specific C-to-G base editing activity.
URI
https://pr.ibs.re.kr/handle/8788114/10735
DOI
10.1038/s41587-021-00943-2
ISSN
1087-0156
Appears in Collections:
Center for Genome Engineering(유전체 교정 연구단) > 1. Journal Papers (저널논문)
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