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Disabled infectious single cycle-herpes simplex virus (DISC-HSV) as a vector for immunogene therapy of cancer.
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2002
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VaccinationCancer-associated VirusViral PersistenceEfficient Delivery SystemNeurovirologyDisc-hsv-mgm-csf VectorImmunologyAntiviral ResponseTherapeutic VaccineVirologyHerpesvirusesRapid Gene ExpressionVaccine DesignImmunotherapyMedicineViral OncologyImmunogene TherapyHerpes Simplex Virus Vaccines
Disabled infectious single cycle-herpes simplex viruses (DISC-HSV) have been shown to be safe for use in humans and may be considered efficacious as vectors for immunogene therapy in cancer. Preclinical studies show that DISC-HSV is an efficient delivery system for cytokine genes and antigens. DISC-HSV infects a high proportion of cells, resulting in rapid gene expression for at least 72 h. The DISC-HSV-mGM-CSF vector, when inoculated into tumors, induces tumor regression in a high percentage of animals, concomitant with establishing a cytotoxic T-cell response, which is MHC class I restricted and directed against peptides of known tumor antigens. The inherent properties of DISC-HSV makes it a suitable vector for consideration in human immunogene therapy trials.