Lung cancer patients' CD4+ T cells are activated in vitro by MHC II cell-based vaccines despite the presence of myeloid-derived suppressor cells

MK Srivastava, JJ Bosch, JA Thompson… - Cancer Immunology …, 2008 - Springer
MK Srivastava, JJ Bosch, JA Thompson, BR Ksander, MJ Edelman, S Ostrand-Rosenberg
Cancer Immunology, Immunotherapy, 2008Springer
Background Advanced non-small cell lung cancer (NSCLC) remains an incurable disease.
Immunotherapies that activate patients' T cells against resident tumor cells are being
developed; however, these approaches may not be effective in NSCLC patients due to
tumor-induced immune suppression. A major cause of immune suppression is myeloid-
derived suppressor cells (MDSC). Because of the strategic role of CD4+ T lymphocytes in
the activation of cytotoxic CD8+ T cells and immune memory, we are developing cell-based …
Background
Advanced non-small cell lung cancer (NSCLC) remains an incurable disease. Immunotherapies that activate patients’ T cells against resident tumor cells are being developed; however, these approaches may not be effective in NSCLC patients due to tumor-induced immune suppression. A major cause of immune suppression is myeloid-derived suppressor cells (MDSC). Because of the strategic role of CD4+ T lymphocytes in the activation of cytotoxic CD8+ T cells and immune memory, we are developing cell-based vaccines that activate tumor-specific CD4+ T cells in the presence of MDSC. The vaccines are NSCLC cell lines transfected with costimulatory (CD80) plus major histocompatibility complex class II (MHC II) genes that are syngeneic to the recipient. The absence of invariant chain promotes the presentation of endogenously synthesized tumor antigens, and the activation of MHC II-restricted, tumor-antigen-specific CD4+ T cells.
Methods
Potential vaccine efficacy was tested in vitro by priming and boosting peripheral blood mononuclear cells from ten NSCLC patients who had varying levels of MDSC. CD4+ T cell activation was quantified by measuring Type 1 and Type 2 cytokine release.
Results
The vaccines activated CD4+ T cells from all ten patients, despite the presence of CD33+CD11b+ MDSC. Activated CD4+ T cells were specific for NSCLC and did not cross-react with tumor cells derived from non-lung tissue or normal lung fibroblasts.
Conclusions
The NSCLC vaccines activate tumor-specific CD4+ T cells in the presence of potent immune suppression, and may be useful for the treatment of patients with NSCLC.
Springer