CDK12 loss drives prostate cancer progression, transcription-replication conflicts, and synthetic lethality with paralog CDK13.

IF 11.7 1区 医学 Q1 CELL BIOLOGY
Cell Reports Medicine Pub Date : 2024-10-15 Epub Date: 2024-10-04 DOI:10.1016/j.xcrm.2024.101758
Jean Ching-Yi Tien, Jie Luo, Yu Chang, Yuping Zhang, Yunhui Cheng, Xiaoju Wang, Jianzhang Yang, Rahul Mannan, Somnath Mahapatra, Palak Shah, Xiao-Ming Wang, Abigail J Todd, Sanjana Eyunni, Caleb Cheng, Ryan J Rebernick, Lanbo Xiao, Yi Bao, James Neiswender, Rachel Brough, Stephen J Pettitt, Xuhong Cao, Stephanie J Miner, Licheng Zhou, Yi-Mi Wu, Estefania Labanca, Yuzhuo Wang, Abhijit Parolia, Marcin Cieslik, Dan R Robinson, Zhen Wang, Felix Y Feng, Jonathan Chou, Christopher J Lord, Ke Ding, Arul M Chinnaiyan
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引用次数: 0

Abstract

Biallelic loss of cyclin-dependent kinase 12 (CDK12) defines a metastatic castration-resistant prostate cancer (mCRPC) subtype. It remains unclear, however, whether CDK12 loss drives prostate cancer (PCa) development or uncovers pharmacologic vulnerabilities. Here, we show Cdk12 ablation in murine prostate epithelium is sufficient to induce preneoplastic lesions with lymphocytic infiltration. In allograft-based CRISPR screening, Cdk12 loss associates positively with Trp53 inactivation but negatively with Pten inactivation. Moreover, concurrent Cdk12/Trp53 ablation promotes proliferation of prostate-derived organoids, while Cdk12 knockout in Pten-null mice abrogates prostate tumor growth. In syngeneic systems, Cdk12/Trp53-null allografts exhibit luminal morphology and immune checkpoint blockade sensitivity. Mechanistically, Cdk12 inactivation mediates genomic instability by inducing transcription-replication conflicts. Strikingly, CDK12-mutant organoids and patient-derived xenografts are sensitive to inhibition or degradation of the paralog kinase, CDK13. We therein establish CDK12 as a bona fide tumor suppressor, mechanistically define how CDK12 inactivation causes genomic instability, and advance a therapeutic strategy for CDK12-mutant mCRPC.

CDK12 的缺失会导致前列腺癌进展、转录-复制冲突以及与同系物 CDK13 的合成致死。
细胞周期蛋白依赖性激酶 12(CDK12)的双叶缺失定义了一种转移性去势抵抗性前列腺癌(mCRPC)亚型。然而,CDK12 的缺失是否会导致前列腺癌(PCa)的发展或揭示药理学上的弱点,目前仍不清楚。在这里,我们展示了小鼠前列腺上皮细胞中的 CDK12 消减足以诱发淋巴细胞浸润的肿瘤前病变。在基于CRISPR的异体移植筛选中,Cdk12的缺失与Trp53失活呈正相关,但与Pten失活呈负相关。此外,Cdk12/Trp53同时消减会促进前列腺衍生组织细胞的增殖,而在Pten无效的小鼠中敲除Cdk12会抑制前列腺肿瘤的生长。在合成系统中,Cdk12/Trp53 缺失的异体移植物表现出腔内形态和免疫检查点阻断敏感性。从机理上讲,Cdk12失活通过诱导转录-复制冲突来介导基因组不稳定性。令人震惊的是,CDK12突变的器官组织和患者衍生的异种移植物对CDK13旁系激酶的抑制或降解很敏感。我们在其中确立了 CDK12 作为真正的肿瘤抑制因子的地位,从机理上定义了 CDK12 失活如何导致基因组不稳定,并推进了 CDK12 突变 mCRPC 的治疗策略。
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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来源期刊
Cell Reports Medicine
Cell Reports Medicine Biochemistry, Genetics and Molecular Biology-Biochemistry, Genetics and Molecular Biology (all)
CiteScore
15.00
自引率
1.40%
发文量
231
审稿时长
40 days
期刊介绍: Cell Reports Medicine is an esteemed open-access journal by Cell Press that publishes groundbreaking research in translational and clinical biomedical sciences, influencing human health and medicine. Our journal ensures wide visibility and accessibility, reaching scientists and clinicians across various medical disciplines. We publish original research that spans from intriguing human biology concepts to all aspects of clinical work. We encourage submissions that introduce innovative ideas, forging new paths in clinical research and practice. We also welcome studies that provide vital information, enhancing our understanding of current standards of care in diagnosis, treatment, and prognosis. This encompasses translational studies, clinical trials (including long-term follow-ups), genomics, biomarker discovery, and technological advancements that contribute to diagnostics, treatment, and healthcare. Additionally, studies based on vertebrate model organisms are within the scope of the journal, as long as they directly relate to human health and disease.
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