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Improvement of TaC9-ABE mediated correction of human SMN2 gene

Biotechnol Bioeng. 2024-06; 
Xiaohua Peng, Yue Chi, Jinling Wang, Shuangpeng Li, Yang Liu, Chengcheng Tang, Xiaoqing Zhou, Xuan Lu, Yue Gao, Liangxue Lai, Min Chen, Qingjian Zou
Products/Services Used Details Operation
Catalog Gene Editing … -Cas9-NLS Nuclease (GenScript) and two sgRNAs (target specific locus 5′-attttgtctgaaaccctgta-3′ and 5′-tcagatgttaaaaagttgaa-3′, GenScript) were mixed and electroporated into … Get A Quote

Abstract

Spinal muscular atrophy (SMA) is a devastating neuromuscular disease caused by mutations in the survival motor neuron 1 (SMN1) gene. Gene editing technology repairs the conversion of the 6th base T to C in exon 7 of the paralogous SMN2 gene, compensating for the SMN protein expression and promoting the survival and function of motor neurons. However, low editing efficiency and unintended off-target effects limit the application of this technology. Here, we optimized a TaC9-adenine base editor (ABE) system by combining Cas9 nickase with the transcription activator-like effector (TALE)-adenosine deaminase fusion protein to effectively and precisely edit SMN2 without detectable Cas9 dependent off-target effects in... More

Keywords

Cas9 nickase, adenine base editor, induced pluripotent stem cells, spinal muscular atrophy, survival motor neuron gene, transcription activator‐like effector