Inhibition of Activated/Memory (CD45RO+) T Cells by Oxidative Stress Associated with Block of NF-κB Activation

Abstract

Impaired immune responses in cancer patients have been associated with oxidative stress. Increased levels of reactive oxygen species released from activated, tumor-infiltrating macrophages or granulocytes may therefore constitute a hurdle for effective immunotherapy against cancer. In this study, we investigated functional consequences and molecular events in T cells exposed to low levels of oxidative stress. We observed that cytokine production of human PBMC, upon stimulation with an HLA-A*0201-restricted influenza peptide and nonspecific receptor cross-linking, was reduced after exposure to micromolar levels of H₂O₂. Functional impairment as measured by IFN-γ release occurred earlier and at lower doses of exogenously added H₂O₂ than required to induce apoptosis. This suggests that there is a dose window of oxidative stress leading to T cell unresponsiveness in the absence of apoptosis. The reduction of Th1 cytokines, induced by H₂O₂, was predominantly observed in memory/effector (CD45RO⁺) T cells and correlated with a block in NF-κB activation. IL-10 production was more profoundly influenced by low doses of H₂O₂ than IFN-γ, TNF-α, and IL-2. The influence of H₂O₂ on production of IL-10 was not significantly different between memory/activated and naive T cells. These observations suggest that Th1 and Th2 cytokines are differently regulated under conditions of oxidative stress. Taken together, these findings may explain why Ag-experienced, CD45RO⁺, T cells found in the tumor milieu are functionally suppressed.