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    Curr Gene Ther. 2011 Feb;11(1):11-27.

    Meganucleases and other tools for targeted genome engineering: perspectives and challenges for gene therapy.

    Source

    Cellectis Genome Surgery, 102 Avenue Gaston Roussel, Romainville Cedex, France.

    Abstract

    The importance of safer approaches for gene therapy has been underscored by a series of severe adverse events (SAEs) observed in patients involved in clinical trials for Severe Combined Immune Deficiency Disease (SCID) and Chromic Granulomatous Disease (CGD). While a new generation of viral vectors is in the process of replacing the classical gamma-retrovirus-based approach, a number of strategies have emerged based on non-viral vectorization and/or targeted insertion aimed at achieving safer gene transfer. Currently, these methods display lower efficacies than viral transduction although many of them can yield more than 1% of engineered cells in vitro. Nuclease-based approaches, wherein an endonuclease is used to trigger site-specific genome editing, can significantly increase the percentage of targeted cells. These methods therefore provide a real alternative to classical gene transfer as well as gene editing. However, the first endonuclease to be in clinic today is not used for gene transfer, but to inactivate a gene (CCR5) required for HIV infection. Here, we review these alternative approaches, with a special emphasis on meganucleases, a family of naturally occurring rare-cutting endonucleases, and speculate on their current and future potential.

    PMID:
    21182466
    [PubMed - indexed for MEDLINE]
    PMCID:
    PMC3267165
    Free PMC Article

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