PRMT1-mediated modification of H4R3me2a promotes liver cancer progression by enhancing the transcriptional activity of SOX18.

IF 5.6 2区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY

Hepatology Communications Pub Date : 2025-03-24 eCollection Date: 2025-04-01 DOI:10.1097/HC9.0000000000000647

Jing Ling, Siying Wang, Chenhe Yi, Xingling Zheng, Yangyang Zhou, Shunjia Lou, Haoyu Li, Ruobing Yu, Wei Wu, Qiangxin Wu, Xiaoxiao Sun, Yuanyuan Lv, Huijue Zhu, Qi Li, Haojie Jin, Jinhong Chen, Jiaojiao Zheng, Wenxin Qin

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引用次数: 0

Abstract

Background: HCC is one of the most prevalent and deadliest malignancies worldwide, with a poor prognosis. Altered histone modifications have been shown to play a significant role in HCC. However, the biological roles and clinical relevance of specific histone modifications, such as the asymmetric dimethylation on arginine 3 of histone H4 (H4R3me2a), remain poorly understood in HCC.

Methods: In this study, immunohistochemical staining was performed to assess histone H4R3me2a modification in 32 pairs of HCC tissues and corresponding adjacent nontumor liver tissues. Cellular-level experiments and subcutaneous xenograft models in nude mice were used to investigate the effects of silencing protein arginine methyltransferase 1 (PRMT1) with shRNA or pharmacologically blocking PRMT1 activity on HCC cell proliferation, migration, and invasion. RNA-seq analysis combined with Chip-qPCR validation was employed to explore the regulatory mechanism of PRMT1 on SOX18 expression. The downstream target of SOX18 was identified using the JASPAR database and a dual-luciferase reporter system.

Results: The level of histone H4R3me2a modification was significantly elevated in HCC tissues and closely associated with poor prognosis in patients with HCC. Silencing PRMT1 or pharmacologically inhibiting its activity effectively suppressed the proliferation, migration, and invasion of HCC cells. Mechanistically, PRMT1 was found to regulate SOX18 expression by modulating histone H4R3me2a modification in the SOX18 promoter region. LOXL1 was identified as a downstream target of the transcription factor SOX18.

Conclusions: This study revealed the clinical relevance of histone H4R3me2a modification in HCC and demonstrated that PRMT1 promotes malignant behavior in HCC cells by modulating H4R3me2a modification in the SOX18 promoter region. The findings elucidate the role and molecular mechanism of PRMT1-mediated histone H4R3me2a modification in HCC progression and highlight the potential clinical applications of PRMT1 inhibitors. These results may provide new insights into the treatment of HCC.

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prmt1介导的H4R3me2a修饰通过增强SOX18的转录活性促进肝癌进展。

背景：HCC是世界范围内最常见和最致命的恶性肿瘤之一，预后较差。组蛋白修饰的改变已被证明在HCC中起重要作用。然而，特定组蛋白修饰的生物学作用和临床相关性，如组蛋白H4 （H4R3me2a）精氨酸3上的不对称二甲基化，在HCC中的作用仍然知之甚少。方法：本研究采用免疫组化染色法对32对HCC组织及相应的邻近非肿瘤肝组织进行组蛋白H4R3me2a修饰评价。通过细胞水平实验和裸鼠皮下异种移植模型，研究用shRNA沉默蛋白精氨酸甲基转移酶1 （PRMT1）或药理学阻断PRMT1活性对HCC细胞增殖、迁移和侵袭的影响。采用RNA-seq分析结合Chip-qPCR验证，探讨PRMT1对SOX18表达的调控机制。利用JASPAR数据库和双荧光素酶报告系统鉴定SOX18的下游靶点。结果：组蛋白H4R3me2a修饰水平在HCC组织中显著升高，与HCC患者预后不良密切相关。沉默PRMT1或通过药物抑制其活性可有效抑制HCC细胞的增殖、迁移和侵袭。在机制上，PRMT1通过调节SOX18启动子区域组蛋白H4R3me2a修饰来调节SOX18的表达。LOXL1被鉴定为转录因子SOX18的下游靶点。结论：本研究揭示了组蛋白H4R3me2a修饰在HCC中的临床意义，并证明PRMT1通过调节SOX18启动子区H4R3me2a修饰促进HCC细胞的恶性行为。这些发现阐明了PRMT1介导的组蛋白H4R3me2a修饰在HCC进展中的作用和分子机制，并强调了PRMT1抑制剂的潜在临床应用。这些结果可能为HCC的治疗提供新的见解。

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

Hepatology Communications GASTROENTEROLOGY & HEPATOLOGY-

CiteScore

8.00

自引率

2.00%

发文量

248

审稿时长

8 weeks

期刊介绍： Hepatology Communications is a peer-reviewed, online-only, open access journal for fast dissemination of high quality basic, translational, and clinical research in hepatology. Hepatology Communications maintains high standard and rigorous peer review. Because of its open access nature, authors retain the copyright to their works, all articles are immediately available and free to read and share, and it is fully compliant with funder and institutional mandates. The journal is committed to fast publication and author satisfaction.