Targeting RBM39 through indisulam induced mis-splicing of mRNA to exert anti-cancer effects in T-cell acute lymphoblastic leukemia.

IF 11.4 1区医学 Q1 ONCOLOGY

Journal of Experimental & Clinical Cancer Research Pub Date : 2024-07-24 DOI:10.1186/s13046-024-03130-8

Tongting Ji, Yang Yang, Juanjuan Yu, Hongli Yin, Xinran Chu, Pengju Yang, Ling Xu, Xiaodong Wang, Shaoyan Hu, Yizhen Li, Xiaochen Wu, Wengyuan Liu, Bi Zhou, Wenjuan Wang, Shuqi Zhang, Wei Cheng, Yanling Chen, Lei Shi, Zhiheng Li, Ran Zhuo, Yongping Zhang, Yanfang Tao, Di Wu, Xiaolu Li, Zimu Zhang, Jun-Jie Fan, Jian Pan, Jun Lu

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引用次数: 0

Abstract

Background: Despite the use of targeted therapeutic approaches, T-cell acute lymphoblastic leukemia (T-ALL) is still associated with a high incidence of complications and a poor prognosis. Indisulam (also known as E7070), a newly identified molecular glue compound, has demonstrated increased therapeutic efficacy in several types of cancer through the rapid degradation of RBM39. This study aimed to evaluate the therapeutic potential of indisulam in T-ALL, elucidate its underlying mechanisms and explore the role of the RBM39 gene.

Methods: We verified the anticancer effects of indisulam in both in vivo and in vitro models. Additionally, the construction of RBM39-knockdown cell lines using shRNA confirmed that the malignant phenotype of T-ALL cells was dependent on RBM39. Through RNA sequencing, we identified indisulam-induced splicing anomalies, and proteomic analysis helped pinpoint protein changes caused by the drug. Comprehensive cross-analysis of these findings facilitated the identification of downstream effectors and subsequent validation of their functional roles.

Results: Indisulam has significant antineoplastic effects on T-ALL. It attenuates cell proliferation, promotes apoptosis and interferes with cell cycle progression in vitro while facilitating tumor remission in T-ALL in vivo models. This investigation provides evidence that the downregulation of RBM39 results in the restricted proliferation of T-ALL cells both in vitro and in vivo, suggesting that RBM39 is a potential target for T-ALL treatment. Indisulam's efficacy is attributed to its ability to induce RBM39 degradation, causing widespread aberrant splicing and abnormal translation of the critical downstream effector protein, THOC1, ultimately leading to protein depletion. Moreover, the presence of DCAF15 is regarded as critical for the effectiveness of indisulam, and its absence negates the ability of indisulam to induce the desired functional alterations.

Conclusion: Our study revealed that indisulam, which targets RBM39 to induce tumor cell apoptosis, is an effective drug for treating T-ALL. Targeting RBM39 through indisulam leads to mis-splicing of pre-mRNAs, resulting in the loss of key effectors such as THOC1.

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通过茚虫威诱导 mRNA 的错误拼接来靶向 RBM39，从而在 T 细胞急性淋巴细胞白血病中发挥抗癌作用。

背景：尽管使用了靶向治疗方法，但T细胞急性淋巴细胞白血病（T-ALL）的并发症发生率仍然很高，预后较差。茚地舒兰（又称 E7070）是一种新发现的分子胶化合物，它通过快速降解 RBM39 而提高了对多种类型癌症的疗效。本研究旨在评估茚地舒兰在T-ALL中的治疗潜力，阐明其潜在机制，并探索RBM39基因的作用：我们在体内和体外模型中验证了茚虫威的抗癌作用。此外，利用 shRNA 构建的 RBM39 敲除细胞系证实了 T-ALL 细胞的恶性表型依赖于 RBM39。通过RNA测序，我们发现了茚地舒兰诱导的剪接异常，而蛋白质组分析则有助于确定药物引起的蛋白质变化。对这些发现的综合交叉分析有助于确定下游效应因子，并随后验证其功能作用：结果：吲哚舒兰对 T-ALL 有显著的抗肿瘤作用。结果：茚地舒兰对T-ALL具有显著的抗肿瘤作用，它能在体外抑制细胞增殖、促进细胞凋亡并干扰细胞周期的进展，同时在体内T-ALL模型中促进肿瘤缓解。这项研究提供的证据表明，下调 RBM39 会导致 T-ALL 细胞在体外和体内增殖受限，这表明 RBM39 是治疗 T-ALL 的潜在靶点。茚虫威的疗效归功于其诱导 RBM39 降解的能力，这种降解会引起广泛的剪接异常和关键下游效应蛋白 THOC1 的翻译异常，最终导致蛋白耗竭。此外，DCAF15的存在被认为是茚虫威有效性的关键，它的缺失否定了茚虫威诱导所需的功能改变的能力：我们的研究表明，茚虫威靶向RBM39诱导肿瘤细胞凋亡，是治疗T-ALL的有效药物。通过茚虫威靶向 RBM39 会导致前 mRNA 的错误拼接，从而导致 THOC1 等关键效应因子的缺失。

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

Journal of Experimental & Clinical Cancer Research 医学-肿瘤学

CiteScore

18.20

自引率

1.80%

发文量

333

审稿时长

1 months

期刊介绍： The Journal of Experimental & Clinical Cancer Research is an esteemed peer-reviewed publication that focuses on cancer research, encompassing everything from fundamental discoveries to practical applications. We welcome submissions that showcase groundbreaking advancements in the field of cancer research, especially those that bridge the gap between laboratory findings and clinical implementation. Our goal is to foster a deeper understanding of cancer, improve prevention and detection strategies, facilitate accurate diagnosis, and enhance treatment options. We are particularly interested in manuscripts that shed light on the mechanisms behind the development and progression of cancer, including metastasis. Additionally, we encourage submissions that explore molecular alterations or biomarkers that can help predict the efficacy of different treatments or identify drug resistance. Translational research related to targeted therapies, personalized medicine, tumor immunotherapy, and innovative approaches applicable to clinical investigations are also of great interest to us. We provide a platform for the dissemination of large-scale molecular characterizations of human tumors and encourage researchers to share their insights, discoveries, and methodologies with the wider scientific community. By publishing high-quality research articles, reviews, and commentaries, the Journal of Experimental & Clinical Cancer Research strives to contribute to the continuous improvement of cancer care and make a meaningful impact on patients' lives.