Hypoxia enhances immunosuppression by inhibiting CD4+ effector T cell function and promoting Treg activity

AM Westendorf, K Skibbe, A Adamczyk… - Cellular Physiology and …, 2017 - karger.com
AM Westendorf, K Skibbe, A Adamczyk, J Buer, R Geffers, W Hansen, E Pastille…
Cellular Physiology and Biochemistry, 2017karger.com
Abstract Background/Aims: Hypoxia occurs in many pathological conditions, including
inflammation and cancer. Within this context, hypoxia was shown to inhibit but also to
promote T cell responses. Due to this controversial function, we aimed to explore whether an
insufficient anti-tumour response during colitis-associated colon cancer could be ascribed to
a hypoxic microenvironment. Methods: Colitis-associated colon cancer was induced in
wildtype mice, and hypoxia as well as T cell immunity were analysed in the colonic tumour …
Abstract
Background/Aims: Hypoxia occurs in many pathological conditions, including inflammation and cancer. Within this context, hypoxia was shown to inhibit but also to promote T cell responses. Due to this controversial function, we aimed to explore whether an insufficient anti-tumour response during colitis-associated colon cancer could be ascribed to a hypoxic microenvironment. Methods: Colitis-associated colon cancer was induced in wildtype mice, and hypoxia as well as T cell immunity were analysed in the colonic tumour tissues. In addition, CD4+ effector T cells and regulatory T cells were cultured under normoxic and hypoxic conditions and examined regarding their phenotype and function. Results: We observed severe hypoxia in the colon of mice suffering from colitis-associated colon cancer that was accompanied by a reduced differentiation of CD4+ effector T cells and an enhanced number and suppressive activity of regulatory T cells. Complementary ex vivo and in vitro studies revealed that T cell stimulation under hypoxic conditions inhibited the differentiation, proliferation and IFN-γ production of TH1 cells and enhanced the suppressive capacity of regulatory T cells. Moreover, we identified an active role for HIF-1α in the modulation of CD4+ T cell functions under hypoxic conditions. Conclusion: Our data indicate that oxygen availability can function as a local modulator of CD4+ T cell responses and thus influences tumour immune surveillance in inflammation-associated colon cancer.
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