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Transduction of fetal mice with a feline lentiviral vector induces liver tumors which exhibit an E2F activation signature.


ABSTRACT: Lentiviral vectors are widely used in basic research and clinical applications for gene transfer and long-term expression; however, safety issues have not yet been completely resolved. In this study, we characterized hepatocarcinomas that developed in mice 1 year after in utero administration of a feline-derived lentiviral vector. Mapped viral integration sites differed among tumors and did not coincide with the regions of chromosomal aberrations. Furthermore, gene expression profiling revealed that no known cancer-associated genes were deregulated in the vicinity of viral integrations. Nevertheless, five of the six tumors exhibited highly significant upregulation of E2F target genes, of which a majority are associated with oncogenesis, DNA damage response, and chromosomal instability. We further show in vivo and in vitro that E2F activation occurs early on following transduction of both fetal mice and cultured human hepatocytes. On the basis of the similarities in E2F target gene expression patterns among tumors and the lack of evidence implicating insertional mutagenesis, we propose that transduction of fetal mice with a feline lentiviral vector induces E2F-mediated major cellular processes that drive hepatocytes toward uncontrolled proliferation culminating in tumorigenesis.

SUBMITTER: Condiotti R 

PROVIDER: S-EPMC3978808 | biostudies-literature | 2014 Jan

REPOSITORIES: biostudies-literature

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Transduction of fetal mice with a feline lentiviral vector induces liver tumors which exhibit an E2F activation signature.

Condiotti Reba R   Goldenberg Daniel D   Giladi Hilla H   Schnitzer-Perlman Temima T   Waddington Simon N SN   Buckley Suzanne Mk SM   Heim Denise D   Cheung Wing W   Themis Matthew M   Coutelle Charles C   Simerzin Alina A   Osejindu Emma E   Wege Henning H   Themis Michael M   Galun Eithan E  

Molecular therapy : the journal of the American Society of Gene Therapy 20130828 1


Lentiviral vectors are widely used in basic research and clinical applications for gene transfer and long-term expression; however, safety issues have not yet been completely resolved. In this study, we characterized hepatocarcinomas that developed in mice 1 year after in utero administration of a feline-derived lentiviral vector. Mapped viral integration sites differed among tumors and did not coincide with the regions of chromosomal aberrations. Furthermore, gene expression profiling revealed  ...[more]

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