Upregulation of CENPM is associated with poor clinical outcome and suppression of immune profile in clear cell renal cell carcinoma.

IF 2.7 3区 生物学
Zhi-Cheng Zhang, Yi-Fu Liu, Ping Xi, Ye-Chen Nie, Ting Sun, Bin-Bin Gong
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引用次数: 0

Abstract

Background: The response of advanced clear cell renal cell carcinoma (ccRCC) to immunotherapy is still not durable, suggesting that the immune landscape of ccRCC still needs to be refined, especially as some molecules that have synergistic effects with immune checkpoint genes need to be explored.

Methods: The expression levels of CENPM and its relationship with clinicopathological features were explored using the ccRCC dataset from TCGA and GEO databases. Quantitative polymerase chain reaction (qPCR) analysis was performed to validate the expression of CENPM in renal cancer cell lines. Kaplan-Meier analysis, COX regression analysis and Nomogram construction were used to systematically evaluate the prognostic potential of CENPM in ccRCC. Besides, single gene correlation analysis, protein-protein interaction (PPI) network, genetic ontology (GO), kyoto encyclopedia of genes and genomes (KEGG) and gene set enrichment analysis (GSEA) were used to predict the biological behaviour of CENPM and the possible signalling pathways involved. Finally, a comprehensive analysis of the crosstalk between CENPM and immune features in the tumor microenvironment was performed based on the ssGSEA algorithm, the tumor immune dysfunction and exclusion (TIDE) algorithm, the TIMER2.0 database and the TISIDB database.

Results: CENPM was significantly upregulated in ccRCC tissues and renal cancer cell lines and was closely associated with poor clinicopathological features and prognosis. Pathway enrichment analysis revealed that CENPM may be involved in the regulation of the cell cycle in ccRCC and may have some crosstalk with the immune microenvironment in tumors. The ssGSEA algorithm, CIBERSOPT algorithm suggests that CENPM is associated with suppressor immune cells in ccRCC such as regulatory T cells. The ssGSEA algorithm, CIBERSOPT algorithm suggests that CENPM is associated with suppressor immune cells in ccRCC such as regulatory T cells. Furthermore, the TISIDB database provides evidence that not only CENPM is positively associated with immune checkpoint genes such as CTLA4, PDCD1, LAG3, TIGIT, but also chemokines and receptors (such as CCL5, CXCL13, CXCR3, CXCR5) may be responsible for the malignant phenotype of CENPM in ccRCC. Meanwhile, predictions based on the TIDE algorithm support that patients with high CENPM expression have a worse response to immunotherapy.

Conclusions: The upregulation of CENPM in ccRCC predicts a poor clinical outcome, and this malignant phenotype may be associated with its exacerbation of the immunosuppressive state in the tumor microenvironment.

Abstract Image

Abstract Image

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在透明细胞肾细胞癌中,CENPM的上调与临床预后差和免疫谱抑制有关。
背景:晚期透明细胞肾细胞癌(ccRCC)对免疫治疗的反应仍然不持久,提示ccRCC的免疫景观仍然需要完善,特别是需要探索一些与免疫检查点基因具有协同作用的分子。方法:利用TCGA和GEO数据库的ccRCC数据集,探讨CENPM的表达水平及其与临床病理特征的关系。采用定量聚合酶链反应(qPCR)验证了CENPM在肾癌细胞系中的表达。应用Kaplan-Meier分析、COX回归分析和Nomogram construct分析系统评价CENPM在ccRCC中的预后潜力。此外,通过单基因相关分析、蛋白-蛋白相互作用(PPI)网络、遗传本体论(GO)、京都基因基因组百科全书(KEGG)和基因集富集分析(GSEA)预测了CENPM的生物学行为和可能参与的信号通路。最后,基于ssGSEA算法、肿瘤免疫功能障碍与排斥(TIDE)算法、TIMER2.0数据库和TISIDB数据库,对肿瘤微环境中CENPM与免疫特征之间的串扰进行综合分析。结果:CENPM在ccRCC组织和肾癌细胞系中表达显著上调,并与不良的临床病理特征和预后密切相关。通路富集分析显示,CENPM可能参与ccRCC细胞周期的调控,并可能与肿瘤免疫微环境存在一定的串扰。ssGSEA算法、CIBERSOPT算法提示CENPM与ccRCC中的抑制性免疫细胞(如调节性T细胞)相关。ssGSEA算法、CIBERSOPT算法提示CENPM与ccRCC中的抑制性免疫细胞(如调节性T细胞)相关。此外,TISIDB数据库提供的证据表明,不仅CENPM与免疫检查点基因(如CTLA4、PDCD1、LAG3、TIGIT)呈正相关,而且趋化因子和受体(如CCL5、CXCL13、CXCR3、CXCR5)也可能导致ccRCC中CENPM的恶性表型。同时,基于TIDE算法的预测支持高CENPM表达的患者对免疫治疗的反应较差。结论:ccRCC中CENPM的上调预示着不良的临床预后,这种恶性表型可能与其肿瘤微环境中免疫抑制状态的加剧有关。
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来源期刊
Hereditas
Hereditas Biochemistry, Genetics and Molecular Biology-Genetics
CiteScore
3.80
自引率
3.70%
发文量
0
期刊介绍: For almost a century, Hereditas has published original cutting-edge research and reviews. As the Official journal of the Mendelian Society of Lund, the journal welcomes research from across all areas of genetics and genomics. Topics of interest include human and medical genetics, animal and plant genetics, microbial genetics, agriculture and bioinformatics.
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