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CD4+ T helper 2 cell–macrophage crosstalk induces IL-24–mediated breast cancer suppression
Bo Wang, Yun Xia, Can Zhou, Yuhan Zeng, Heehwa G. Son, Shadmehr Demehri
Bo Wang, Yun Xia, Can Zhou, Yuhan Zeng, Heehwa G. Son, Shadmehr Demehri
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Research Article Immunology Oncology

CD4+ T helper 2 cell–macrophage crosstalk induces IL-24–mediated breast cancer suppression

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Abstract

CD4+ T cells contribute to antitumor immunity and are implicated in the efficacy of cancer immunotherapies. In particular, CD4+ T helper 2 (Th2) cells were recently found to block spontaneous breast carcinogenesis. However, the antitumor potential of Th2 cells in targeting established breast cancer remains uncertain. Herein, we demonstrate that Th2 cells induced by the topical calcipotriol/thymic stromal lymphopoietin cytokine axis suppressed the growth of established mammary tumors in mice. Interleukin-24 (IL-24), an anticancer cytokine, was highly upregulated in macrophages infiltrating calcipotriol-treated mammary tumors. Macrophages expressed IL-24 in response to IL-4 signaling in combination with Toll-like receptor 4 (TLR4) agonists (e.g., HMGB1) in vitro. Calcipotriol treatment significantly increased HMGB1 release by tumor cells in vivo. CD4+ T cell depletion reduced HMGB1 and IL-24 expression, reversing calcipotriol’s therapeutic efficacy. Macrophage depletion and TLR4 inhibition also reduced the therapeutic efficacy of calcipotriol. Importantly, calcipotriol treatment failed to control mammary tumors lacking the IL-24 receptor on tumor cells. Collectively, our findings reveal that Th2 cell–macrophage crosstalk leads to IL-24–mediated tumor cell death, highlighting a promising therapeutic strategy to tackle breast cancer.

Authors

Bo Wang, Yun Xia, Can Zhou, Yuhan Zeng, Heehwa G. Son, Shadmehr Demehri

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Figure 5

Deletion of the IL-24 receptor in tumor cells blocks the antitumor effect of calcipotriol on mammary tumors.

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Deletion of the IL-24 receptor in tumor cells blocks the antitumor effec...
(A) Representative IF images of IL-24, IL-22Rα, and cleaved caspase-3–stained PyMt mammary tumor in calcipotriol-treated WT mice. Dotted circles outline a tumor focus. (B) Schematic diagram of the experimental setup to assess the contribution of the IL-24/IL-20R axis to the efficacy of topical calcipotriol treatment against PyMt mammary tumor growth. (C) Representative macroscopic images of WT and Il20rb–/– PyMt mammary tumors in WT mice (dotted circles highlight the tumor sites). (D and E) WT versus Il20rb–/– PyMt mammary tumor volume over time in calcipotriol-treated WT mice presented as (D) mean tumor volumes + SD and (E) spider plot (n = 10 in each group). Two-way ANOVA (D and E). Scale bars: 100 μm (A) and 1 cm (C).

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