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High-fidelity Cas13 variants for targeted RNA degradation with minimal collateral effects.
Tong, Huawei; Huang, Jia; Xiao, Qingquan; He, Bingbing; Dong, Xue; Liu, Yuanhua; Yang, Xiali; Han, Dingyi; Wang, Zikang; Wang, Xuchen; Ying, Wenqin; Zhang, Runze; Wei, Yu; Xu, Chunlong; Zhou, Yingsi; Li, Yanfei; Cai, Minqing; Wang, Qifang; Xue, Mingxing; Li, Guoling; Fang, Kailun; Zhang, Hainan; Yang, Hui.
Nat Biotechnol ; 2022 Aug 11.
Article in English | MEDLINE | ID: covidwho-1996868

ABSTRACT

CRISPR-Cas13 systems have recently been used for targeted RNA degradation in various organisms. However, collateral degradation of bystander RNAs has limited their in vivo applications. Here, we design a dual-fluorescence reporter system for detecting collateral effects and screening Cas13 variants in mammalian cells. Among over 200 engineered variants, several Cas13 variants including Cas13d and Cas13X exhibit efficient on-target activity but markedly reduced collateral activity. Furthermore, transcriptome-wide off-targets and cell growth arrest induced by Cas13 are absent for these variants. High-fidelity Cas13 variants show similar RNA knockdown activity to wild-type Cas13 but no detectable collateral damage in transgenic mice or adeno-associated-virus-mediated somatic cell targeting. Thus, high-fidelity Cas13 variants with minimal collateral effects are now available for targeted degradation of RNAs in basic research and therapeutic applications.

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