FOXA1 overexpression suppresses interferon signaling and immune response in cancer
Yundong He, Liguo Wang, Ting Wei, Yu-Tian Xiao, Haoyue Sheng, Hengchuan Su, Daniel P. Hollern, Xiaoling Zhang, Jian Ma, Simeng Wen, Hongyan Xie, Yuqian Yan, Yunqian Pan, Xiaonan Hou, Xiaojia Tang, Vera J. Suman, Jodi M. Carter, Richard Weinshilboum, Liewei Wang, Krishna R. Kalari, Saravut J. Weroha, Alan H. Bryce, Judy C. Boughey, Haidong Dong, Charles M. Perou, Dingwei Ye, Matthew P. Goetz, Shancheng Ren, Haojie Huang
Yundong He, Liguo Wang, Ting Wei, Yu-Tian Xiao, Haoyue Sheng, Hengchuan Su, Daniel P. Hollern, Xiaoling Zhang, Jian Ma, Simeng Wen, Hongyan Xie, Yuqian Yan, Yunqian Pan, Xiaonan Hou, Xiaojia Tang, Vera J. Suman, Jodi M. Carter, Richard Weinshilboum, Liewei Wang, Krishna R. Kalari, Saravut J. Weroha, Alan H. Bryce, Judy C. Boughey, Haidong Dong, Charles M. Perou, Dingwei Ye, Matthew P. Goetz, Shancheng Ren, Haojie Huang
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Research Article Cell biology

FOXA1 overexpression suppresses interferon signaling and immune response in cancer

Abstract

Androgen receptor–positive prostate cancer (PCa) and estrogen receptor–positive luminal breast cancer (BCa) are generally less responsive to immunotherapy compared with certain tumor types such as melanoma. However, the underlying mechanisms are not fully elucidated. In this study, we found that FOXA1 overexpression inversely correlated with interferon (IFN) signature and antigen presentation gene expression in PCa and BCa patients. FOXA1 bound the STAT2 DNA-binding domain and suppressed STAT2 DNA-binding activity, IFN signaling gene expression, and cancer immune response independently of the transactivation activity of FOXA1 and its mutations detected in PCa and BCa. Increased FOXA1 expression promoted cancer immuno- and chemotherapy resistance in mice and PCa and BCa patients. These findings were also validated in bladder cancer expressing high levels of FOXA1. FOXA1 overexpression could be a prognostic factor to predict therapy resistance and a viable target to sensitize luminal PCa, BCa, and bladder cancer to immuno- and chemotherapy.

Authors

Yundong He, Liguo Wang, Ting Wei, Yu-Tian Xiao, Haoyue Sheng, Hengchuan Su, Daniel P. Hollern, Xiaoling Zhang, Jian Ma, Simeng Wen, Hongyan Xie, Yuqian Yan, Yunqian Pan, Xiaonan Hou, Xiaojia Tang, Vera J. Suman, Jodi M. Carter, Richard Weinshilboum, Liewei Wang, Krishna R. Kalari, Saravut J. Weroha, Alan H. Bryce, Judy C. Boughey, Haidong Dong, Charles M. Perou, Dingwei Ye, Matthew P. Goetz, Shancheng Ren, Haojie Huang

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Figure 6

Foxa1 knockdown sensitizes murine PCa to anti–PD-1 and anti-CTLA4 combination therapy.

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Foxa1 knockdown sensitizes murine PCa to anti–PD-1 and anti-CTLA4 combin...
(A) Western blot analysis of indicated proteins in MyC-CaP murine PCa cells stably expressing doxycycline-inducible lentiviral shFoxa1#1 (MyC-CaPIN-shFoxa1#1) and treated with or without doxycycline (Dox) or/and IFN-α. Erk2 served as a loading control. (B) Schematic diagram of generation and anti–PD-1/anti-CTLA4 treatment of MyC-CaPIN-shFoxa1#1 prostate tumors in syngeneic mice. Dox, without doxycycline treatment; Dox+, with doxycycline treatment; FCA, flow cytometric analysis; IFC, immunofluorescent cytochemistry. (C and D) Growth of MyC-CaPIN-shFoxa1#1 prostate tumors treated with IgG or combination of anti–PD-1/anti-CTLA4 at the indicated time points (arrowheads) in FVB mice (n = 10 mice/group). Statistical significance was determined by 2-way ANOVA. (E) Tumor-free survival of syngeneic mice bearing MyC-CaPIN-shFoxa1#1 prostate tumors treated with IgG or anti–PD-1/anti-CTLA4 (n = 10 mice/group). Statistical significance was determined by log-rank (Mantel-Cox) test. (F) Flow cytometric analysis of Foxa1-, CD8-, and Gzmb-positive cells in MyC-CaPIN-shFoxa1#1 tumors from mice 2 days after the last administration of IgG or anti–PD-1/anti-CTLA4. Data are shown in the bar graphs as mean ± SD (n = 5 mice/group). Statistical significance was determined by 1-way ANOVA with Bonferroni’s correction for multiple tests. (G) RT-qPCR analysis of Foxa1 and murine Stat2 target genes Isg15, Ifi44, H2-k1, and Psmb9 in MyC-CaPIN-shFoxa1#1 tumors from mice 2 days after the last administration of IgG or anti–PD-1/anti-CTLA4. The data are presented as the mean ± SD (n = 5 mice/group). Statistical significance was determined by 1-way ANOVA with Bonferroni’s correction for multiple tests.