Targeting ADAR1 with a small molecule for the treatment of prostate cancer

Xiao Wang; Jiaxing Li; Yasheng Zhu; Hongtao Shen; Jiayu Ding; Ting Zeng; Wenjian Min; Shun Qing Liang; Lei Huang; Zhongrui Shi; Hao Shen; Fei Huang; Kai Yuan; Wenbin Kuang; Minghui Ji; Chengliang Sun; Yi Hou; Liping Wang; Weijiao Chen; Yuzhang Jiang; Haiping Hao; Yibei Xiao; Peng Yang

doi:10.1038/s43018-025-00907-4

Targeting ADAR1 with a small molecule for the treatment of prostate cancer

Xiao Wang, Jiaxing Li, Yasheng Zhu, Hongtao Shen, Jiayu Ding, Ting Zeng, Wenjian Min, Shun Qing Liang, Lei Huang, Zhongrui Shi, Hao Shen, Fei Huang, Kai Yuan, Wenbin Kuang, Minghui Ji, Chengliang Sun, Yi Hou, Liping Wang, Weijiao Chen, Yuzhang JiangHaiping Hao, Yibei Xiao, Peng Yang

Medicine - Gastro, Hepatology, Nutrition Division

Research output: Contribution to journal › Article › peer-review

6 Scopus citations

Abstract

Despite the initial response to androgen signaling therapy, most cases of prostate cancer (PCa) eventually relapse and remain incurable. The specific function of ADAR1 that governs PCa progression and specific inhibitors of ADAR are underexplored. In this study, we demonstrate that highly expressed ADAR1 is a crucial oncogenic target in PCa and develop an effective small-molecule ADAR1 inhibitor, ZYS-1, with marked antitumor efficacy and a favorable safety profile. Either genetic or pharmacological inhibition of ADAR1 dramatically suppressed PCa growth and metastasis and potentiated the antitumor immune response. Moreover, ZYS-1 can enhance the antitumor effect of immunotherapy. We also reveal that ADAR1 represses the translation of MTDH in an editing-dependent manner, which drives cell proliferation and invasion in PCa. Collectively, our findings suggest that ADAR1 is a druggable target in PCa and highlight the widespread applicability of ADAR1 inhibitors for a broad spectrum of malignancies.

Original language	English (US)
Article number	5450
Pages (from-to)	474-492
Number of pages	19
Journal	Nature Cancer
Volume	6
Issue number	3
DOIs	https://doi.org/10.1038/s43018-025-00907-4
State	Published - Mar 2025

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© The Author(s), under exclusive licence to Springer Nature America, Inc. 2025.

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Wang, X., Li, J., Zhu, Y., Shen, H., Ding, J., Zeng, T., Min, W., Liang, S. Q., Huang, L., Shi, Z., Shen, H., Huang, F., Yuan, K., Kuang, W., Ji, M., Sun, C., Hou, Y., Wang, L., Chen, W., ... Yang, P. (2025). Targeting ADAR1 with a small molecule for the treatment of prostate cancer. Nature Cancer, 6(3), 474-492. Article 5450. https://doi.org/10.1038/s43018-025-00907-4

Wang, X, Li, J, Zhu, Y, Shen, H, Ding, J, Zeng, T, Min, W, Liang, SQ, Huang, L, Shi, Z, Shen, H, Huang, F, Yuan, K, Kuang, W, Ji, M, Sun, C, Hou, Y, Wang, L, Chen, W, Jiang, Y, Hao, H, Xiao, Y & Yang, P 2025, 'Targeting ADAR1 with a small molecule for the treatment of prostate cancer', Nature Cancer, vol. 6, no. 3, 5450, pp. 474-492. https://doi.org/10.1038/s43018-025-00907-4

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abstract = "Despite the initial response to androgen signaling therapy, most cases of prostate cancer (PCa) eventually relapse and remain incurable. The specific function of ADAR1 that governs PCa progression and specific inhibitors of ADAR are underexplored. In this study, we demonstrate that highly expressed ADAR1 is a crucial oncogenic target in PCa and develop an effective small-molecule ADAR1 inhibitor, ZYS-1, with marked antitumor efficacy and a favorable safety profile. Either genetic or pharmacological inhibition of ADAR1 dramatically suppressed PCa growth and metastasis and potentiated the antitumor immune response. Moreover, ZYS-1 can enhance the antitumor effect of immunotherapy. We also reveal that ADAR1 represses the translation of MTDH in an editing-dependent manner, which drives cell proliferation and invasion in PCa. Collectively, our findings suggest that ADAR1 is a druggable target in PCa and highlight the widespread applicability of ADAR1 inhibitors for a broad spectrum of malignancies.",

author = "Xiao Wang and Jiaxing Li and Yasheng Zhu and Hongtao Shen and Jiayu Ding and Ting Zeng and Wenjian Min and Liang, \{Shun Qing\} and Lei Huang and Zhongrui Shi and Hao Shen and Fei Huang and Kai Yuan and Wenbin Kuang and Minghui Ji and Chengliang Sun and Yi Hou and Liping Wang and Weijiao Chen and Yuzhang Jiang and Haiping Hao and Yibei Xiao and Peng Yang",

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AU - Wang, Xiao

AU - Li, Jiaxing

AU - Zhu, Yasheng

AU - Shen, Hongtao

AU - Ding, Jiayu

AU - Zeng, Ting

AU - Min, Wenjian

AU - Liang, Shun Qing

AU - Huang, Lei

AU - Shi, Zhongrui

AU - Shen, Hao

AU - Huang, Fei

AU - Yuan, Kai

AU - Kuang, Wenbin

AU - Ji, Minghui

AU - Sun, Chengliang

AU - Hou, Yi

AU - Wang, Liping

AU - Chen, Weijiao

AU - Jiang, Yuzhang

AU - Hao, Haiping

AU - Xiao, Yibei

AU - Yang, Peng

PY - 2025/3

Y1 - 2025/3

N2 - Despite the initial response to androgen signaling therapy, most cases of prostate cancer (PCa) eventually relapse and remain incurable. The specific function of ADAR1 that governs PCa progression and specific inhibitors of ADAR are underexplored. In this study, we demonstrate that highly expressed ADAR1 is a crucial oncogenic target in PCa and develop an effective small-molecule ADAR1 inhibitor, ZYS-1, with marked antitumor efficacy and a favorable safety profile. Either genetic or pharmacological inhibition of ADAR1 dramatically suppressed PCa growth and metastasis and potentiated the antitumor immune response. Moreover, ZYS-1 can enhance the antitumor effect of immunotherapy. We also reveal that ADAR1 represses the translation of MTDH in an editing-dependent manner, which drives cell proliferation and invasion in PCa. Collectively, our findings suggest that ADAR1 is a druggable target in PCa and highlight the widespread applicability of ADAR1 inhibitors for a broad spectrum of malignancies.

AB - Despite the initial response to androgen signaling therapy, most cases of prostate cancer (PCa) eventually relapse and remain incurable. The specific function of ADAR1 that governs PCa progression and specific inhibitors of ADAR are underexplored. In this study, we demonstrate that highly expressed ADAR1 is a crucial oncogenic target in PCa and develop an effective small-molecule ADAR1 inhibitor, ZYS-1, with marked antitumor efficacy and a favorable safety profile. Either genetic or pharmacological inhibition of ADAR1 dramatically suppressed PCa growth and metastasis and potentiated the antitumor immune response. Moreover, ZYS-1 can enhance the antitumor effect of immunotherapy. We also reveal that ADAR1 represses the translation of MTDH in an editing-dependent manner, which drives cell proliferation and invasion in PCa. Collectively, our findings suggest that ADAR1 is a druggable target in PCa and highlight the widespread applicability of ADAR1 inhibitors for a broad spectrum of malignancies.

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Targeting ADAR1 with a small molecule for the treatment of prostate cancer

Abstract

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UN SDGs

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