Generation and validation of a Leber Congenital Amaurosis, Type 12 patient-specific iPSC line (LVPEIi006-B) with a splice-site mutation in RD3 and an isogenic mutation-corrected iPSC line (LVPEIi006-B-1)
IF 0.8
4区 医学
Q4 BIOTECHNOLOGY & APPLIED MICROBIOLOGY
引用次数: 0
Abstract
Leber congenital amaurosis, Type 12 is an early onset, autosomal recessive retinal disease caused by mutations in RD3. We report the generation of a patient-specific iPSC line (LVPEIi006-B), using Sendai viral vector-based reprogramming approach and an isogenic, mutation-corrected iPSC line (LVPEIi006-B-1), using an en31FnCas9-based adenine base editor (ABE) system. Both lines were clonally expanded and genotyped to confirm the presence of patient-specific mutation and desired base correction in the edited line. Both lines maintained their stemness, pluripotency, genomic integrity and could differentiate into retinal organoids. The mutation-corrected, heterozygous iPSC-derived retinal organoids displayed a partial restoration of normal RD3 mRNA splicing.
勒伯先天性无视力症 12 型是一种由 RD3 基因突变引起的早发性常染色体隐性视网膜疾病。我们报告了利用基于仙台病毒载体的重编程方法产生的患者特异性 iPSC 株系(LVPEIi006-B),以及利用基于 en31FnCas9 的腺嘌呤碱基编辑器(ABE)系统产生的同源、突变校正 iPSC 株系(LVPEIi006-B-1)。这两个品系都进行了克隆扩增和基因分型,以确认编辑品系中存在患者特异性突变和所需的碱基校正。两个品系都保持了干性、多能性和基因组完整性,并能分化成视网膜器官组织。经过突变校正的杂合子iPSC衍生视网膜器官组织部分恢复了正常的RD3 mRNA剪接。
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来源期刊
Stem cell research
生物-生物工程与应用微生物
CiteScore
2.20
自引率
8.30%
发文量
338
审稿时长
55 days
期刊介绍:
Stem Cell Research is dedicated to publishing high-quality manuscripts focusing on the biology and applications of stem cell research. Submissions to Stem Cell Research, may cover all aspects of stem cells, including embryonic stem cells, tissue-specific stem cells, cancer stem cells, developmental studies, stem cell genomes, and translational research. Stem Cell Research publishes 6 issues a year.
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