Cas9-mediated replacement of expanded CAG repeats in a pig model of Huntington’s disease

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简介:

  • 作者: Sen Yan, Xiao Zheng, Yingqi Lin, Caijuan Li, Zhaoming Liu, Jiawei Li, Zhuchi Tu, Yu Zhao, Chunhui Huang, Yizhi Chen, Jun Li, Xichen Song, Bofeng Han, Wei Wang, Weien Liang, Liangxue Lai, Xiao-Jiang Li & Shihua Li
  • 杂志: Nature Biomedical Engineering
  • Doi: https://www.doi.org/10.1038/s41551-023-01007-3
  • 出版日期: 2023 Feb 16

论文中使用的产品/服务

Quotation shows PackGene:The AAV-mini-cmv-spCas9(AAV9-Cas9, AAV-Cas9), AAV-controlgRNA- RFP (AAV9-Ctrl-gRNA-RFP, AAV9-Ctrl-gRNA, Ctrl-gRNA) and AAV9-HTT-gRNA-RFP-20Q (AAV9-HTT-gRNA-20Q, HTT-gRNA-20Q) donor vectors were sent to PackGene Biotech for viral packaging and production.

Research Field:CNS

AAV Serotype:AAV9

Animal or cell line strain:3-month-old piglets

询价

摘要

The monogenic nature of Huntington’s disease (HD) and other neurodegenerative diseases caused by the expansion of glutamine-encoding CAG repeats makes them particularly amenable to gene therapy. Here we show the feasibility of replacing expanded CAG repeats in the mutant HTT allele with a normal CAG repeat in genetically engineered pigs mimicking the selective neurodegeneration seen in patients with HD. A single intracranial or intravenous injection of adeno-associated virus encoding for Cas9, a single-guide RNA targeting the HTT gene, and donor DNA containing the normal CAG repeat led to the depletion of mutant HTT in the animals and to substantial reductions in the dysregulated expression and neurotoxicity of mutant HTT and in neurological symptoms. Our findings support the further translational development of virally delivered Cas9-based gene therapies for the treatment of genetic neurodegenerative diseases.

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