miRNA-503 inhibition exerts anticancer effects and reduces tumor growth in mesothelioma.

IF 11.4 1区医学 Q1 ONCOLOGY

Journal of Experimental & Clinical Cancer Research Pub Date : 2025-02-22 DOI:10.1186/s13046-025-03283-0

Miriam Piccioni, Francesco Di Meo, Anna Valentino, Virginia Campani, Maddalena Arigoni, Mirella Tanori, Mariateresa Mancuso, Rossana Cuciniello, Marco Tomasetti, Federica Monaco, Gaia Goteri, Enrico P Spugnini, Raffaele A Calogero, Giuseppe De Rosa, Gianfranco Peluso, Alfonso Baldi, Stefania Crispi

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引用次数: 0

Abstract

Background: Malignant mesothelioma (MM) is a rare and aggressive form of cancer that affects the mesothelial surfaces, associated with exposure to asbestos fibres. To date, no cure is available for MM and therapeutically approved treatments are based on the use of platinum compounds often used in combination with other drugs. We have previously analysed the efficacy of a cisplatin/piroxicam (CDDP/P) combined treatment showing that this treatment was able to reduce in vivo tumor growth. Several studies reported that platinum-drug sensitivity in cancer is connected to modulation of the expression of non-coding RNAs. In this study we analysed if the CDDP/P treatment was able to modulate miRNAs expression in MM.

Methods: miRNA sequencing performed on MSTO-211 H cells treated with CDDP with CDDP/P led us to identify miRNA-503 - downregulated by CDDP/P - as a novel miRNA that acts as an oncomiR in MM. The effect of miRNA-503 inhibition was evaluated in vitro in mesothelioma cells analysing apoptosis induction and reduction of cancer properties. Inhibition of miR-503 expression in vivo, was analysed in ectopic mouse model of MM by using LNP encapsulating anti-mir-503 and miR-503 expression was evaluated in human MM samples.

Results: In vitro and in vivo analysis confirmed miR-503 acts as oncogene in MM since its inhibition was able to reduce cell cancer properties and tumor growth in ectopic mouse model of MM. Its expression was found upregulated in human MM patients compared to normal pleura. Bioinformatic analysis indicated BTG1, CCNG1, EDG1, and TIMP2 as putative target genes of miRNA-503. These genes showed an opposite expression compared to miR-503 levels both in cells and in MM samples. Finally, microarray analysis indicated that miR-503 inhibition affected the expression of the well-known MM biomarkers: CXCL8, SERPINE1 and Osteopontin.

Conclusions: Our study is the first reporting an oncomiR role for miR-503 in MM and suggests that its inactivation could have a clinical value in MM patients. This study reveals that miRNA-503 acts as an oncomiR in MM suggesting that its inhibition, through LNP delivery, has the potential to be considered as a novel therapeutic strategy in MM.

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背景：恶性间皮瘤（MM）是一种罕见的侵袭性癌症，影响间皮细胞表面，与接触石棉纤维有关。迄今为止，恶性间皮瘤尚无根治方法，经批准的治疗方法以使用铂化合物为基础，通常与其他药物联合使用。我们以前分析过顺铂/吡罗昔康（CDDP/P）联合治疗的疗效，结果显示这种治疗方法能够减少体内肿瘤的生长。一些研究报告指出，癌症患者对铂类药物的敏感性与非编码 RNA 的表达调节有关。在这项研究中，我们分析了 CDDP/P 治疗是否能调节 MM 中 miRNAs 的表达。方法：对用 CDDP 和 CDDP/P 治疗的 MSTO-211 H 细胞进行 miRNA 测序，结果发现，CDDP/P 下调的 miRNA-503 是一种新型的 miRNA，它在 MM 中起着 oncomiR 的作用。我们在间皮瘤细胞中对抑制 miRNA-503 的效果进行了体外评估，分析了诱导细胞凋亡和减少癌症特性的作用。在MM的异位小鼠模型中，使用包裹抗mir-503的LNP分析了体内抑制miR-503表达的情况，并在人类MM样本中评估了miR-503的表达情况：结果：体外和体内分析证实了miR-503在MM中的致癌作用，因为抑制miR-503能降低异位小鼠MM模型的细胞癌特性和肿瘤生长。与正常胸膜相比，miR-503在人类MM患者中表达上调。生物信息学分析表明，BTG1、CCNG1、EDG1 和 TIMP2 是 miRNA-503 的假定靶基因。这些基因在细胞和 MM 样本中的表达与 miR-503 水平相反。最后，微阵列分析表明，抑制 miR-503 会影响著名 MM 生物标志物的表达：结论：我们的研究首次报道了miR-503在MM中的作用，并表明抑制miR-503可能对MM患者有临床价值。这项研究揭示了 miRNA-503 在 MM 中的作用，表明通过 LNP 递送抑制 miRNA-503 有可能被视为 MM 的一种新型治疗策略。

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

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.