多路复用
基因组编辑
计算生物学
清脆的
生物
基因组
基因
遗传学
胞苷
生物化学
酶
作者
Wenhui Zhang,Tomomi Aida,Ricardo C.H. del Rosario,Jonathan J. Wilde,Chenhui Ding,Xiaohui Zhang,Zulqarnain Baloch,Yan Huang,Yu Tang,Duanduan Li,Hongyu Lu,Yang Zhou,Minqing Jiang,Dongdong Xu,Zhihao Fang,Zhan-Hong Zheng,Qunshan Huang,Guoping Feng,Shihua Yang
标识
DOI:10.1038/s41467-020-16173-0
摘要
Abstract Common polygenic diseases result from compounded risk contributed by multiple genetic variants, meaning that simultaneous correction or introduction of single nucleotide variants is required for disease modeling and gene therapy. Here, we show precise, efficient, and simultaneous multiplex base editing of up to three target sites across 11 genes/loci in cynomolgus monkey embryos using CRISPR-based cytidine- and adenine-base editors. Unbiased whole genome sequencing demonstrates high specificity of base editing in monkey embryos. Our data demonstrate feasibility of multiplex base editing for polygenic disease modeling in primate zygotes.
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