Platinum-based drugs disrupt STAT6-mediated suppression of immune responses against cancer in humans and mice
W. Joost Lesterhuis, … , Carl G. Figdor, I. Jolanda M. de Vries
W. Joost Lesterhuis, … , Carl G. Figdor, I. Jolanda M. de Vries
Published July 18, 2011
Citation Information: J Clin Invest. 2011;121(8):3100-3108. https://doi.org/10.1172/JCI43656.
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Research Article Oncology

Platinum-based drugs disrupt STAT6-mediated suppression of immune responses against cancer in humans and mice

Abstract

Tumor microenvironments feature immune inhibitory mechanisms that prevent T cells from generating effective antitumor immune responses. Therapeutic interventions aimed at disrupting these inhibitory mechanisms have been shown to enhance antitumor immunity, but they lack direct cytotoxic effects. Here, we investigated the effect of cytotoxic cancer chemotherapeutics on immune inhibitory pathways. We observed that exposure to platinum-based chemotherapeutics markedly reduced expression of the T cell inhibitory molecule programmed death receptor-ligand 2 (PD-L2) on both human DCs and human tumor cells. Downregulation of PD-L2 resulted in enhanced antigen-specific proliferation and Th1 cytokine secretion as well as enhanced recognition of tumor cells by T cells. Further analysis revealed that STAT6 controlled downregulation of PD-L2. Consistent with these data, patients with STAT6-expressing head and neck cancer displayed enhanced recurrence-free survival upon treatment with cisplatin-based chemoradiation compared with patients with STAT6-negative tumors, demonstrating the clinical relevance of platinum-induced STAT6 modulation. We therefore conclude that platinum-based anticancer drugs can enhance the immunostimulatory potential of DCs and decrease the immunosuppressive capability of tumor cells. This dual action of platinum compounds may extend their therapeutic application in cancer patients and provides a rationale for their use in combination with immunostimulatory compounds.

Authors

W. Joost Lesterhuis, Cornelis J.A. Punt, Stanleyson V. Hato, Dagmar Eleveld-Trancikova, Bastiaan J.H. Jansen, Stefan Nierkens, Gerty Schreibelt, Annemiek de Boer, Carla M.L. Van Herpen, Johannes H. Kaanders, Johan H.J.M. van Krieken, Gosse J. Adema, Carl G. Figdor, I. Jolanda M. de Vries

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Figure 5

Enhanced T cell activation by DCs upon platinum exposure is mediated through STAT6 dephosphorylation.

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Enhanced T cell activation by DCs upon platinum exposure is mediated thr...
(A) Western blot analysis of cytokine-matured DCs treated for 24 hours with 5 or 7.5 μg/ml cisplatin or oxaliplatin or medium during maturation. Blot lanes were run on the same gel but were noncontiguous (white line). (B) MLR with DCs that were transfected with STAT6 siRNA or control siRNA and subsequently matured with or without 5 μg/ml oxaliplatin. A representative experiment is shown. n = 3. (C) PD-L2 expression of BM-derived CD11c+ IL-4/LPS–stimulated DCs from wild-type and Stat6–/– BALB/c mice, cultured in the presence or absence of cisplatin. Depicted are the normalized MFI and SEM of 1 of 2 independent experiments performed in triplicate. *P < 0.05; ***P < 0.001.