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Active specific T-cell-based immunotherapy for cancer: nucleic acids, peptides, whole native proteins, recombinant viruses, with dendritic cell adjuvants or whole tumor cell-based vaccines. Principles and future prospects.
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1998
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Future ProspectsImmunologyImmunoeditingCd4 T Cell ResponsesImmunotherapeuticsImmune Cell TherapyImmunotherapyTumor BiologySynthetic ImmunologyTumor ImmunologyTumor ImmunityCancer VaccinesCancer ResearchGrowth SuppressionTherapeutic VaccineCell BiologyTumor MicroenvironmentCancer ImmunosurveillanceMouse Tumor ModelsHuman MelanomaImmune Checkpoint InhibitorImmunomodulationDendritic Cell AdjuvantsMedicineNucleic Acids
Whereas tumor cells are poor immunogens, recombinant tumor cells or dendritic cells as well as engineered viruses have been demonstrated to elicit specific antitumor immune responses leading to tumor growth suppression and long-lasting immunity in mouse tumor models. Single cytotoxic T lymphocyte-defined epitope-based strategies have proved useful for immunization in tumor-bearing mice. This strategy is under investigation in human melanoma, along with adjuvants such as cytokines or dendritic cells. Flt3L is an in vivo dendritic-cell growth factor that offers new prospects in the field of active specific immunotherapy. These immunotherapeutic approaches are being tested in clinical trials, and may open up novel avenues for disease-free patients with poor prognostic factors.