miR-466 Contributes to the Enhanced Antitumor Effect of Bortezomib on Non-Small-Cell Lung Cancer by Inhibiting CCND1.

IF 2 4区医学 Q3 ONCOLOGY

Chemotherapy Pub Date : 2022-01-01 Epub Date: 2022-01-18 DOI:10.1159/000518936

Wei-Hua Wang, Jia-Ming Zhan, Yan-Lei Tang, Ning Zhou, Wei-Yan Liu, Dao-Wen Jiang

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引用次数: 4

Abstract

Introduction: Changes in microRNAs (miRs) contribute to the alternative chemo-resistance of cancers. Bortezomib (BTZ) is a well-characterized anticancer agent that inhibits proteasome, and its effect is associated with the function of miRs. Based on the data of microarray assay and comprehensive bioinformatics analyses, in the current study, we explored the role of miR-466 and its downstream effector CCND1 in the BTZ-resistance of non-small-cell lung cancer (NSCLC) cells.

Methods: miR expression profiles in NSCLC tissues and paratumor tissues were determined with microarray assay. The potential miR involved in the chemo-resistance of NSCLC cells was explored via a series of bioinformatics analyses, and miR-466 was selected. Afterward, levels of miR-466 and CCND1 were investigated in NSCLC samples and analyzed by clinicopathologic parameters, including age, sex, stage of NSCLC, tumor size, tumor differentiation status, and lymphocytic infiltration status. The expression of CCND1 and miR-466 was then modulated in vitro to explore the influence on cell phenotypes, which was then verified with mouse models.

Results: Based on microarray detection, 287 miRs were dysexpressed between NSCLC tissues and paratumor tissues, including 90 upregulated members and 197 downregulated members. After bioinformatics analyses and reverse transcription quantitative PCR validation, miR-466 and CCND1 were selected. Following clinical investigations, miR-466 was downregulated, while CCND1 was upregulated in NSCLC samples, contributing to the advanced cancer progression. The overexpression of CCND1 increased cell viability, suppressed cell apoptosis, decreased p21 and induced N-cadherin, CCND2, and CDK4 under BTZ treatment. The induced expression of miR-466 re-sensitized NSCLC cells to BTZ treatment. In the animal model, the overexpression of CCND1 impaired the inhibitory effect of BTZ on the growth and metastasis of solid tumor, which was restored by miR-466 induction.

Conclusion: The findings showed that the interaction between BTZ, miR-466, and CCND1 determined the antitumor effect of BTZ on NSCLC.

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miR-466通过抑制CCND1促进硼替佐米对非小细胞肺癌的抗肿瘤作用

microRNAs (miRs)的变化有助于癌症的替代化疗耐药。硼替佐米(BTZ)是一种典型的抑制蛋白酶体的抗癌药物，其作用与miRs的功能有关。本研究基于微阵列分析和综合生物信息学分析的数据，探讨了miR-466及其下游效应物CCND1在非小细胞肺癌(NSCLC)细胞btz耐药中的作用。方法:采用微阵列法检测miR在非小细胞肺癌组织及肿瘤旁组织中的表达谱。通过一系列生物信息学分析，我们探索了miR参与NSCLC细胞耐药的潜在机制，并选择了miR-466。随后，研究了NSCLC样本中miR-466和CCND1的水平，并通过年龄、性别、NSCLC分期、肿瘤大小、肿瘤分化状态和淋巴细胞浸润状态等临床病理参数进行分析。然后在体外调节CCND1和miR-466的表达，以探索对细胞表型的影响，然后用小鼠模型验证。结果:基于微阵列检测，在NSCLC组织和肿瘤旁组织中有287个miRs表达异常，其中上调成员90个，下调成员197个。经过生物信息学分析和反转录定量PCR验证，选择miR-466和CCND1。经过临床研究，在NSCLC样本中miR-466下调，而CCND1上调，促进了晚期癌症的进展。BTZ处理下，CCND1过表达可提高细胞活力，抑制细胞凋亡，降低p21，诱导N-cadherin、CCND2和CDK4的表达。诱导表达miR-466使NSCLC细胞对BTZ治疗再敏感。在动物模型中，CCND1过表达削弱了BTZ对实体瘤生长和转移的抑制作用，miR-466诱导恢复了BTZ对实体瘤生长和转移的抑制作用。结论:BTZ与miR-466、CCND1的相互作用决定了BTZ对NSCLC的抗肿瘤作用。

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来源期刊

Chemotherapy 医学-药学

CiteScore

5.80

自引率

0.00%

发文量

审稿时长

6-12 weeks

期刊介绍： This journal publishes original research articles and state-of-the-art reviews on all aspects of antimicrobial and antitumor chemotherapy. The results of experimental and clinical investigations into the microbiological and pharmacologic properties of antibacterial, antiviral and antitumor compounds are major topics of publication. Papers selected for the journal offer data concerning the efficacy, toxicology, and interactions of new drugs in single or combined applications. Studies designed to determine the pharmacokinetic and pharmacodynamics properties of similar preparations and comparing their efficacy are also included. Special emphasis is given to the development of drug-resistance, an increasing problem worldwide.