1. IL-4-transduced tumor cell vaccine induces immunoregulatory type 2 CD8 T lymphocytes that cure lung metastases upon adoptive transfer
- Author
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Rodolfo, M., Zilocchi, C., Accornero, P., Barbara Cappetti, Arioli, I., and Colombo, M. P.
- Subjects
Mice, Knockout ,Mice, Inbred BALB C ,Lung Neoplasms ,Folate Receptors, GPI-Anchored ,Longevity ,Immunology ,Gene Transfer Techniques ,Receptors, Cell Surface ,Cell Communication ,CD8-Positive T-Lymphocytes ,Lymphocyte Activation ,Adoptive Transfer ,Cancer Vaccines ,Killer Cells, Natural ,Mice ,Retroviridae ,T-Lymphocyte Subsets ,Animals ,Cytokines ,Immunology and Allergy ,Female ,Interleukin-4 ,Carrier Proteins ,Granulocytes - Abstract
Vaccinations with tumor cells engineered to produce IL-4 prolonged survival and cured 30% of mice bearing pulmonary metastases, an effect abrogated by in vivo depletion of T cells. Vaccination induced type 2 T cell polarization in both CD4 and CD8 T lymphocyte subsets. We focused on the antitumor activity exerted by type 2 CD8+ T cells (Tc2) activated by IL-4 tumor cell vaccination. Tc2 lymphocytes lacked in vitro tumor cytotoxicity, but released IL-4 upon stimulation with tumor cells, as shown by limiting dilution analysis of the frequencies of tumor-specific pCTL and of CD8 cells producing the cytokine. In vivo fresh purified CD8+ T lymphocytes from IL-4-vaccinated mice eliminated 80–100% of lung metastases when transferred into tumor-bearing mice. CD8+ lymphocytes from IL-4-vaccinated IFN-γ knockout (KO), but not from IL-4 KO, mice cured lung metastases, thus indicating that IL-4 produced by Tc2 cells was instrumental for tumor rejection. The antitumor effect of adoptively transferred Tc2 lymphocytes needed host CD8 T cells and AsGM1 leukocyte populations, and partially granulocytes. These data indicate that Tc2 CD8+ T cells exert immunoregulatory functions and induce tumor rejection through the cooperation of bystander lymphoid effector cells. Tumor eradication is thus not restricted to a type 1 response, but can also be mediated by a type 2 biased T cell response.