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CRISPR-Cas9-AAV versus lentivector transduction for genome modification of X-linked severe combined immunodeficiency hematopoietic stem cells

  1. Author:
    Brault, Julie
    Liu, Taylor
    Liu,Siyuan
    Lawson, Amanda
    Choi, Uimook
    Kozhushko, Nikita
    Bzhilyanskaya, Vera
    Pavel-Dinu, Mara
    Meis, Ronald J
    Eckhaus, Michael A
    Burkett,Sandra
    Bosticardo, Marita
    Kleinstiver, Benjamin P
    Notarangelo, Luigi D
    Lazzarotto, Cicera R
    Tsai, Shengdar Q
    Wu, Xiaolin
    Dahl, Gary A
    Porteus, Matthew H
    Malech, Harry L
    De Ravin, Suk See

  2. Author Address

    Laboratory of Clinical Immunology and Microbiology, National Institute of Allergy and Infectious Diseases (NIAID), National Institutes of Health (NIH), Bethesda, MD, United States., Cancer Research Technology Program, Leidos Biomedical Research Inc., Frederick, MD, United States., Department of Pediatrics, Division of Stem Cell Transplantation and Regenerative Medicine, Stanford University, Palo Alto, CA, United States., Cellscript LLC Inc., Madison, WI, United States., Division of Veterinary Resources, Office of Research Services, National Institutes of Health, Bethesda, MD, United States., Molecular Cytogenetic Core Facility, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Frederick, MD, United States., Center for Genomic Medicine and Department of Pathology, Massachusetts General Hospital, Boston, MA, United States., Department of Pathology, Harvard Medical School, Boston, MA, United States., Department of Hematology, St. Jude Children 39;s Research Hospital, Memphis, TN, United States.,
    1. Year: 2023
    2. Date: Jan 4
    3. Epub Date: 2023 01 04
  2. Journal: Frontiers in Immunology
    1. 13
    2. Pages: 1067417
  4. Type of Article: Article
  5. Article Number: 1067417
  1. Abstract:

    Ex vivo gene therapy for treatment of Inborn errors of Immunity (IEIs) have demonstrated significant clinical benefit in multiple Phase I/II clinical trials. Current approaches rely on engineered retroviral vectors to randomly integrate copy(s) of gene-of-interest in autologous hematopoietic stem/progenitor cells (HSPCs) genome permanently to provide gene function in transduced HSPCs and their progenies. To circumvent concerns related to potential genotoxicities due to the random vector integrations in HSPCs, targeted correction with CRISPR-Cas9-based genome editing offers improved precision for functional correction of multiple IEIs. We compare the two approaches for integration of IL2RG transgene for functional correction of HSPCs from patients with X-linked Severe Combined Immunodeficiency (SCID-X1 or XSCID); delivery via current clinical lentivector (LV)-IL2RG versus targeted insertion (TI) of IL2RG via homology-directed repair (HDR) when using an adeno-associated virus (AAV)-IL2RG donor following double-strand DNA break at the endogenous IL2RG locus. In vitro differentiation of LV- or TI-treated XSCID HSPCs similarly overcome differentiation block into Pre-T-I and Pre-T-II lymphocytes but we observed significantly superior development of NK cells when corrected by TI (40.7% versus 4.1%, p = 0.0099). Transplants into immunodeficient mice demonstrated robust engraftment (8.1% and 23.3% in bone marrow) for LV- and TI-IL2RG HSPCs with efficient T cell development following TI-IL2RG in all four patients' HSPCs. Extensive specificity analysis of CRISPR-Cas9 editing with rhAmpSeq covering 82 predicted off-target sites found no evidence of indels in edited cells before (in vitro) or following transplant, in stark contrast to LV's non-targeted vector integration sites. Together, the improved efficiency and safety of IL2RG correction via CRISPR-Cas9-based TI approach provides a strong rationale for a clinical trial for treatment of XSCID patients. Copyright © 2023 Brault, Liu, Liu, Lawson, Choi, Kozhushko, Bzhilyanskaya, Pavel-Dinu, Meis, Eckhaus, Burkett, Bosticardo, Kleinstiver, Notarangelo, Lazzarotto, Tsai, Wu, Dahl, Porteus, Malech and De Ravin.

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External Sources

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  2. DOI: 10.3389/fimmu.2022.1067417
  3. PMID: 36685559
  4. PMCID: PMC9846165

Library Notes

  1. Fiscal Year: FY2022-2023
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