Inhibition of PRMT5 moderately suppresses prostate cancer growth in vivo but enhances its response to immunotherapy

IF 9.1 1区医学 Q1 ONCOLOGY

Cancer letters Pub Date : 2024-08-31 DOI:10.1016/j.canlet.2024.217214

Qinju He , Yuanzhen Zhang , Wenchao Li , Saisai Chen , Jiangling Xiong , Ruizhe Zhao , Kai Yuan , Qiang Hu , Song Liu , Guozhen Gao , Mark T. Bedford , Dean G. Tang , Bin Xu , Cheng Zou , Dingxiao Zhang

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引用次数: 0

Abstract

Protein arginine methylation is a common post-translational modification (PTM) catalyzed by nine protein arginine methyltransferases (PRMTs). As the major symmetric arginine methyltransferase that methylates both histone and non-histone substrates, PRMT5 plays key roles in a number of biological processes critical for development and tumorigenesis. PRMT5 overexpression has been reported in multiple cancer types including prostate cancer (PCa), but the exact biological and mechanistic understanding of PRMT5 in aggressive PCa remains ill-defined. Here, we show that PRMT5 is upregulated in PCa, correlates with worse patient survival, promotes corrupted RNA splicing, and functionally cooperates with an array of pro-tumorigenic pathways to enhance oncogenesis. PRMT5 inhibition via either genetic knockdown or pharmacological inhibition reduces stemness with paralleled differentiation and arrests cell cycle progression without causing appreciable apoptosis. Strikingly, the severity of antitumor effect of PRMT5 inhibition correlates with disease aggressiveness, with AR⁺ PCa being less affected. Molecular characterization pinpoints MYC, but not (or at least to a lesser degree) AR, as the main partner of PRMT5 to form a positive feedback loop to exacerbate malignancy in both AR⁺ and AR^— PCa cells. Inspired by the surprising finding that PRMT5 negatively correlates with tumor immune infiltration and transcriptionally suppresses an immune-gene program, we further show that although PRMT5 inhibitor (PRMT5i) EPZ015666 or anti-PD-1 immunotherapy alone exhibits limited antitumor effects, combination of PRMT5i with anti-PD-1 displays superior efficacy in inhibiting castration-resistant PCa (CRPC) in vivo. Finally, to expand the potential use of PRMT5i through a synthetic lethality concept, we also perform a global CRISPR/Cas9 knockout screen to unravel that many clinical-grade drugs of known oncogenic pathways can be repurposed to target CRPC when used in combination with PRMT5i at low doses. Collectively, our findings establish a rationale to exploit PRMT5i in combination with immunotherapy or other targeted therapies to treat aggressive PCa.

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抑制 PRMT5 可适度抑制前列腺癌在体内的生长，但会增强其对免疫疗法的反应。

蛋白质精氨酸甲基化是一种常见的翻译后修饰（PTM），由九种蛋白质精氨酸甲基转移酶（PRMTs）催化。作为主要的对称精氨酸甲基转移酶，PRMT5 可将组蛋白和非组蛋白底物甲基化，在许多对发育和肿瘤发生至关重要的生物过程中发挥关键作用。据报道，PRMT5 在包括前列腺癌（PCa）在内的多种癌症类型中都有过表达，但人们对 PRMT5 在侵袭性 PCa 中的确切生物学作用和机理的认识仍不明确。在这里，我们发现 PRMT5 在 PCa 中上调，与患者生存率下降相关，会促进 RNA 剪接的破坏，并与一系列促致癌通路进行功能性合作以增强肿瘤发生。通过基因敲除或药物抑制来抑制PRMT5，可降低干细胞分化，阻止细胞周期进展，但不会导致明显的细胞凋亡。令人震惊的是，PRMT5抑制的抗肿瘤作用的严重程度与疾病的侵袭性相关，AR+ PCa受到的影响较小。分子特征描述指出，MYC，而不是（或至少在较低程度上）AR，是 PRMT5 的主要伙伴，形成正反馈回路，加剧 AR+ 和 AR- PCa 细胞的恶性程度。受PRMT5与肿瘤免疫浸润呈负相关并转录抑制免疫基因程序这一惊人发现的启发，我们进一步发现，虽然PRMT5抑制剂（PRMT5i）EPZ015666或抗PD-1免疫疗法单独使用的抗肿瘤效果有限，但PRMT5i与抗PD-1联合使用可在体内显示出抑制阉割耐药PCa（CRPC）的卓越疗效。最后，为了通过合成致死概念扩大 PRMT5i 的潜在用途，我们还进行了全球 CRISPR/Cas9 基因敲除筛选，发现许多已知致癌通路的临床级药物在与低剂量 PRMT5i 联合使用时，可以重新用于靶向 CRPC。总之，我们的研究结果为利用PRMT5i与免疫疗法或其他靶向疗法联合治疗侵袭性PCa提供了理论依据。

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

Cancer letters 医学-肿瘤学

CiteScore

17.70

自引率

2.10%

发文量

427

审稿时长

15 days

期刊介绍： Cancer Letters is a reputable international journal that serves as a platform for significant and original contributions in cancer research. The journal welcomes both full-length articles and Mini Reviews in the wide-ranging field of basic and translational oncology. Furthermore, it frequently presents Special Issues that shed light on current and topical areas in cancer research. Cancer Letters is highly interested in various fundamental aspects that can cater to a diverse readership. These areas include the molecular genetics and cell biology of cancer, radiation biology, molecular pathology, hormones and cancer, viral oncology, metastasis, and chemoprevention. The journal actively focuses on experimental therapeutics, particularly the advancement of targeted therapies for personalized cancer medicine, such as metronomic chemotherapy. By publishing groundbreaking research and promoting advancements in cancer treatments, Cancer Letters aims to actively contribute to the fight against cancer and the improvement of patient outcomes.