System analysis of VEGFA in renal cell carcinoma: The expression, prognosis, gene regulation network and regulation targets.

IF 2.3 4区 医学 Q3 BIOTECHNOLOGY & APPLIED MICROBIOLOGY
Yongli Situ, Qinying Xu, Li Deng, Yan Zhu, Ruxiu Gao, Lei Lei, Zheng Shao
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引用次数: 14

Abstract

Background: VEGFA is one of the most important regulators of angiogenesis and plays a crucial role in cancer angiogenesis and progression. Recent studies have highlighted a relationship between VEGFA expression and renal cell carcinoma occurrence. However, the expression level, gene regulation network, prognostic value, and target prediction of VEGFA in renal cell carcinoma remain unclear. Therefore, system analysis of the expression, gene regulation network, prognostic value, and target prediction of VEGFA in patients with renal cell carcinoma is of great theoretical significance as there is a clinical demand for the discovery of new renal cell carcinoma treatment targets and strategies to further improve renal cell carcinoma treatment efficacy.

Methods: This study used multiple free online databases, including cBioPortal, TRRUST, GeneMANIA, GEPIA, Metascape, UALCAN, LinkedOmics, Metascape, and TIMER for the abovementioned analysis.

Results: VEGFA was upregulated in patients with kidney renal clear cell carcinoma (KIRC) and kidney chromophobe (KICH), and downregulated in patients with kidney renal papillary cell carcinoma (KIRP). Moreover, genetic alterations of VEGFA were found in patients with renal cell carcinoma as follows: 4% (KIRC), 8% (KICH), and 4% (KIRP). The promoter methylation of VEGFA was lower and higher in patients with clinical stages of KIRC and stage 1 KIRP, respectively. VEGFA expression significantly correlated with KIRC and KIRP pathological stages. Furthermore, patients with KICH and KIRP having low VEGFA expression levels had a longer survival than those having high VEGFA expression levels. VEGFA and its neighboring genes functioned in the regulation of protein methylation and glycosylation, as well as muscle fiber growth and differentiation in patients with renal cell carcinoma. Gene Ontology enrichment analysis revealed that the functions of VEGFA and its neighboring genes in patients with renal cell carcinoma are mainly related to cell adhesion molecule binding, catalytic activity, acting on RNA, ATPase activity, actin filament binding, protease binding, transcription coactivator activity, cysteine-type peptidase activity, and calmodulin binding. Transcription factor targets of VEGFA and its neighboring genes in patients with renal cell carcinoma were found: HIF1A, TFAP2A, and ESR1 in KIRC; STAT3, NFKB1, and HIPK2 in KICH; and FOXO3, TFAP2A, and ETS1 in KIRP. We further explored the VEGFA-associated kinase (ATM in KICH as well as CDK1 and AURKB in KIRP) and VEGFA-associated microRNA (miRNA) targets (MIR-21 in KICH as well as MIR-213, MIR-383, and MIR-492 in KIRP). Furthermore, the following genes had the strongest correlation with VEGFA expression in patients with renal cell carcinoma: NOTCH4, GPR4, and TRIB2 in KIRC; CKMT2, RRAGD, and PPARGC1A in KICH; and FLT1, C6orf223, and ESM1 in KIRP. VEGFA expression in patients with renal cell carcinoma was positively associated with immune cell infiltration, including CD8+T cells, CD4+T cells, macrophages, neutrophils, and dendritic cells.

Conclusions: This study revealed VEGFA expression and potential gene regulatory network in patients with renal cell carcinoma, thereby laying a foundation for further research on the role of VEGFA in renal cell carcinoma occurrence. Moreover, the study provides new renal cell carcinoma therapeutic targets and prognostic biomarkers as a reference for fundamental and clinical research.

肾细胞癌中VEGFA的系统分析:表达、预后、基因调控网络及调控靶点。
背景:VEGFA是最重要的血管生成调节因子之一,在肿瘤血管生成和进展中起着至关重要的作用。最近的研究强调了VEGFA表达与肾细胞癌发生之间的关系。然而,VEGFA在肾细胞癌中的表达水平、基因调控网络、预后价值、靶点预测等仍不清楚。因此,系统分析VEGFA在肾癌患者中的表达、基因调控网络、预后价值及靶点预测具有重要的理论意义,临床需要发现新的肾癌治疗靶点和策略,进一步提高肾癌的治疗效果。方法:本研究使用cbiopportal、trust、GeneMANIA、GEPIA、metscape、UALCAN、LinkedOmics、metscape、TIMER等多个免费在线数据库进行上述分析。结果:VEGFA在肾透明细胞癌(KIRC)和肾憎色细胞癌(KICH)患者中表达上调,在肾乳头状细胞癌(KIRP)患者中表达下调。此外,肾癌患者中VEGFA的遗传改变如下:4% (KIRC), 8% (KICH)和4% (KIRP)。在KIRC临床分期和1期KIRP患者中,VEGFA启动子甲基化程度分别较低和较高。VEGFA表达与KIRC、KIRP病理分期有显著相关性。此外,VEGFA表达水平低的KICH和KIRP患者比VEGFA表达水平高的患者生存时间更长。VEGFA及其邻近基因在肾细胞癌患者中调控蛋白甲基化和糖基化,以及肌纤维的生长和分化。基因本体富集分析显示,肾癌患者VEGFA及其邻近基因的功能主要与细胞粘附分子结合、催化活性、作用于RNA、atp酶活性、肌动蛋白丝结合、蛋白酶结合、转录辅激活子活性、半胱氨酸型肽酶活性、钙调素结合等有关。在肾癌患者中发现VEGFA及其邻近基因的转录因子靶点:KIRC中的HIF1A、TFAP2A、ESR1;STAT3、NFKB1和HIPK2在KICH中的作用;FOXO3、TFAP2A和ETS1在KIRP中的表达。我们进一步探索了vegfa相关激酶(KICH中的ATM以及KIRP中的CDK1和AURKB)和vegfa相关的microRNA (miRNA)靶点(KICH中的MIR-21以及KIRP中的MIR-213、MIR-383和MIR-492)。此外,以下基因与肾癌患者VEGFA表达相关性最强:KIRC中的NOTCH4、GPR4、TRIB2;CKMT2、RRAGD和PPARGC1A在KICH中的作用;FLT1、C6orf223和ESM1在KIRP中的表达。肾细胞癌患者的VEGFA表达与免疫细胞浸润呈正相关,包括CD8+T细胞、CD4+T细胞、巨噬细胞、中性粒细胞和树突状细胞。结论:本研究揭示了VEGFA在肾癌患者中的表达及潜在的基因调控网络,为进一步研究VEGFA在肾癌发生中的作用奠定了基础。此外,该研究还提供了新的肾细胞癌治疗靶点和预后生物标志物,为基础和临床研究提供了参考。
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
International Journal of Biological Markers
International Journal of Biological Markers 医学-生物工程与应用微生物
CiteScore
4.10
自引率
0.00%
发文量
43
期刊介绍: IJBM is an international, online only, peer-reviewed Journal, which publishes original research and critical reviews primarily focused on cancer biomarkers. IJBM targets advanced topics regarding the application of biomarkers in oncology and is dedicated to solid tumors in adult subjects. The clinical scenarios of interests are screening and early diagnosis of cancer, prognostic assessment, prediction of the response to and monitoring of treatment.
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