Targeting Ubiquitin-specific Protease 5 Overcomes Chemoresistance via Negatively Regulating p53 in Gastric Cancer.

IF 2.2 4区医学 Q3 MEDICINE, RESEARCH & EXPERIMENTAL

Current molecular medicine Pub Date : 2024-02-09 DOI:10.2174/0115665240278762240202103722

Jing Song, Lei Liu, Fang Wang, Di Bao

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引用次数: 0

Abstract

Background: Resistance to chemotherapy is a major obstacle in the clinical management of gastric cancer, and the mechanisms underlying chemoresistance remain largely unknown.

Aims: This study aimed to investigate the involvement of ubiquitin-specific protease 5 (USP5), a deubiquitinating enzyme, in gastric cancer chemoresistance Methods: USP5 expression was analyzed in fifty paired gastric cancer and adjacent normal tissues, chemo-sensitive and chemo-resistant gastric cancer lines using quantitative ELISA. The role of USP5 was determined using loss-of-function and gainof- function methods. USP5-mediated downstream effectors were analyzed using biochemical methods focusing on p53.

Results: USP5 expression was comparable in tumors and normal in the majority of the cohort. Following chemotherapy treatment, USP5 expression significantly increased in gastric cancer cells, while p53 levels remained unaltered. Overexpression of USP5 amplified growth and migration while decreasing apoptosis induced by serum withdrawal across multiple gastric cancer cell lines. Conversely, USP5 knockdown effectively heightened gastric cancer sensitivity to paclitaxel and 5-FU treatments, particularly targeting chemo-resistant gastric cancer cells by inhibiting proliferation and migration and inducing apoptosis. Additionally, USP5 knockdown increased levels of p53 but not MDM2, increased p53 activity and increased transcription of p53 target genes. In contrast, USP5 overexpression decreased the level and activity of p53 and inhibited transcription of p53 target genes. The anti-proliferative, anti-migratory, and pro-apoptotic effects of USP5 were significantly diminished upon p53 depletion, highlighting the interplay between p53 and USP5 in regulating gastric cancer cell activities. Additionally, USP5 inhibition suppressed chemo-resistant gastric cancer cell migration via suppressing epithelial-mesenchymal transition (EMT) and RhoA activity.

Conclusion: Targeting USP5 inhibition has emerged as a promising alternative therapeutic approach to overcoming chemoresistance in gastric cancer. Additionally, our study sheds light on the novel role of USP5 as a regulator of p53 in gastric cancer.

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通过负调控 p53 靶向泛素特异性蛋白酶 5 克服胃癌的化疗耐药性

背景：目的：本研究旨在探讨泛素特异性蛋白酶 5 (USP5)（一种去泛素化酶）参与胃癌化疗耐药的机制：使用定量酶联免疫吸附分析法分析 50 例配对胃癌和邻近正常组织、化疗敏感和化疗耐药胃癌株中 USP5 的表达。采用功能缺失法和功能增益法确定 USP5 的作用。使用生化方法分析了 USP5 介导的下游效应物，重点是 p53：结果：在大多数样本中，USP5 在肿瘤和正常组织中的表达量相当。化疗后，胃癌细胞中 USP5 的表达明显增加，而 p53 的水平保持不变。在多个胃癌细胞系中，USP5 的过表达会增强细胞的生长和迁移，同时降低血清戒断诱导的细胞凋亡。相反，敲除 USP5 能有效提高胃癌对紫杉醇和 5-FU 治疗的敏感性，尤其是通过抑制增殖和迁移以及诱导凋亡来靶向耐化疗的胃癌细胞。此外，USP5 基因敲除会增加 p53 的水平，但不会增加 MDM2 的水平，提高 p53 的活性并增加 p53 靶基因的转录。相反，过表达 USP5 会降低 p53 的水平和活性，抑制 p53 靶基因的转录。当 p53 缺乏时，USP5 的抗增殖、抗迁移和促凋亡作用会明显减弱，这突显了 p53 和 USP5 在调节胃癌细胞活性方面的相互作用。此外，抑制 USP5 还能通过抑制上皮-间质转化（EMT）和 RhoA 活性抑制耐化疗胃癌细胞的迁移：结论：靶向抑制 USP5 已成为克服胃癌化疗耐药性的一种有前途的替代治疗方法。此外，我们的研究还揭示了 USP5 在胃癌中作为 p53 调节器的新作用。

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

Current molecular medicine 医学-医学：研究与实验

CiteScore

5.00

自引率

4.00%

发文量

141

审稿时长

4-8 weeks

期刊介绍： Current Molecular Medicine is an interdisciplinary journal focused on providing the readership with current and comprehensive reviews/ mini-reviews, original research articles, short communications/letters and drug clinical trial studies on fundamental molecular mechanisms of disease pathogenesis, the development of molecular-diagnosis and/or novel approaches to rational treatment. The reviews should be of significant interest to basic researchers and clinical investigators in molecular medicine. Periodically the journal invites guest editors to devote an issue on a basic research area that shows promise to advance our understanding of the molecular mechanism(s) of a disease or has potential for clinical applications.