RSK1-driven TRIM28/E2F1 feedback loop promotes castration-resistant prostate cancer progression.

The Journal of Clinical Investigation Pub Date : 2025-06-16 DOI:10.1172/jci185119

Miyeong Kim,Jinpeng Liu,Yanquan Zhang,Ruixin Wang,Ryan Goettl,Jennifer Grasso,Derek B Allison,Chi Wang,Tianyan Gao,Xiaoqi Liu,Ka-Wing Fong

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Abstract

Castration-resistant prostate cancer (CRPC) marks the advanced and lethal stage of prostate cancer (PCa). TRIM28, also known as KAP1, is a transcriptional regulator recently shown to promote CRPC cell proliferation and xenograft tumor growth. Nonetheless, knowledge gaps persist regarding the mechanisms underlying TRIM28 upregulation in CRPC as well as the genomic targets regulated by TRIM28. Here, we report that TRIM28 is a E2F1 target in CRPC. Using an integrated genomic approach, we have demonstrated that TRIM28 forms a positive feedback loop to promote the transcriptional activation and genomic function of E2F1 independent of retinoblastoma (Rb) status. Furthermore, we identified RSK1 as a kinase that directly phosphorylates TRIM28 at S473, and, as such, RSK1 drives the TRIM28/E2F1 feedback loop. Accordingly, pS473-TRIM28 promotes CRPC progression, which is mitigated by RSK inhibition. In summary, our study reveals a critical role of the RSK1-TRIM28-E2F1 axis in CRPC progression, which may be exploited as a vulnerability in treating Rb-deficient CRPC.

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rsk1驱动的TRIM28/E2F1反馈回路促进去势抵抗性前列腺癌的进展。

去势抵抗性前列腺癌（CRPC）标志着前列腺癌（PCa）的晚期和致死阶段。TRIM28，也被称为KAP1，是一种转录调节因子，最近被证明可以促进CRPC细胞增殖和异种移植物肿瘤生长。尽管如此，关于TRIM28在CRPC中上调的机制以及TRIM28调控的基因组靶点的知识差距仍然存在。在这里，我们报道TRIM28是CRPC中的E2F1靶点。利用整合的基因组方法，我们已经证明TRIM28形成一个正反馈回路，促进E2F1的转录激活和基因组功能，而不依赖于视网膜母细胞瘤（Rb）状态。此外，我们发现RSK1是一种直接磷酸化TRIM28 S473位点的激酶，因此，RSK1驱动TRIM28/E2F1反馈回路。因此，pS473-TRIM28促进CRPC的进展，而RSK抑制可减轻CRPC的进展。总之，我们的研究揭示了RSK1-TRIM28-E2F1轴在CRPC进展中的关键作用，这可能是治疗rb缺陷CRPC的一个漏洞。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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The Journal of Clinical Investigation

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