A temperature-sensitive and interferon-silent Sendai virus vector for CRISPR-Cas9 delivery and gene editing in primary human cells

Author:

Stevens Christian SORCID,Carmichael JillianORCID,Watkinson Ruth,Kowdle Shreyas,Reis Rebecca A,Hamane Kory,Jang Jason,Park Arnold,Pernet Olivier,Khamaikawin Wannisa,Hong Patrick,Thibault PatriciaORCID,Gowlikar Aditya,An Dong Sung,Lee BenhurORCID

Abstract

ABSTRACTThe transformative potential of gene editing technologies hinges on the development of safe and effective delivery methods. In this study, we developed a temperature-sensitive and interferon-silent Sendai virus (ts SeV) as a novel delivery vector for CRISPR-Cas9 and for efficient gene editing in sensitive human cell types without inducing IFN responses. ts SeV demonstrates unprecedented transduction efficiency in human CD34+ hematopoietic stem and progenitor cells (HSPCs) including transduction of the CD34+/CD38-/CD45RA-/CD90+(Thy1+)/CD49fhighstem cell enriched subpopulation. The frequency ofCCR5editing exceeded 90% and bi-allelicCCR5editing exceeded 70% resulting in significant inhibition of HIV-1 infection in primary human CD14+ monocytes. These results demonstrate the potential of the ts SeV platform as a safe, efficient, and flexible addition to the current gene-editing tool delivery methods, which may help to further expand the possibilities in personalized medicine and the treatment of genetic disorders.

Publisher

Cold Spring Harbor Laboratory

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