Immunotherapy has been effective in many cancer types but has failed in multiple clinical trials in prostate cancers, with the underlying mechanisms remaining largely unclear. Here, we demonstrate that androgen receptor pathway inhibitor (ARPI) plus irradiation (IR) triggered robust anticancer immunity in prostate cancers in both patients and mice. We show that androgen-activated AR suppressed innate immune signaling by inducing inhibitor of nuclear factor kappa-B kinase subunit epsilon (IKBKE) gene repression through HDAC2 interaction with an IKBKE enhancer RNA (IKBKE eRNA, or IKBKE-e). ARPI treatment caused IKBKE derepression and enhanced an IR-induced innate immune response via action of RIG-I and MDA5 dsRNA sensors. IKBKE-e ablation largely enhanced innate immunity in prostate cancer cells in culture and anticancer immunity in mice. Our results revealed AR, HDAC2, and IKBKE eRNA as critical intrinsic immune suppressors in prostate cancer cells, suggesting that rejuvenating inhibitor of nuclear factor kappa-B kinase subunit epsilon (IKKε) signaling by targeting IKBKE-e is an actionable strategy to elicit synthetic anticancer immunity in immunologically "cold" cancers such as prostate cancer.
Reversing enhancer RNA-mediated IKBKE gene repression enables synthetic anticancer immunity in prostate cancer models.
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作者:Li Xiang, Sun Rui, Li Hao, Orme Jacob J, Zhang Xu, Hou Yu, Park Sean S, Zhang Yu, He Yi, Wang Liguo, Rodriguez-Bravo Veronica, Domingo-Domenech Josep, Ren Shancheng, Xia Dan, Fu Guanghou, Jia Zhankui, Huang Haojie
| 期刊: | Journal of Clinical Investigation | 影响因子: | 13.600 |
| 时间: | 2026 | 起止号: | 2026 Jan 16; 136(2):e190928 |
| doi: | 10.1172/JCI190928 | ||
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