Mechanism of atorvastatin in treating hepatocellular carcinoma: a study based on network pharmacology, molecular docking, and bioinformatics analysis.

IF 3.1 4区医学 Q2 PHARMACOLOGY & PHARMACY Naunyn-Schmiedeberg's archives of pharmacology Pub Date : 2025-05-01 Epub Date: 2024-11-28 DOI:10.1007/s00210-024-03598-3

Youwen Hu, Yangyang Xiao

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引用次数: 0

Abstract

Hepatocellular carcinoma (HCC) is a tumor with high morbidity and mortality. Current research suggests that statins may aid in its prevention and treatment, while studies on the associated mechanisms remain limited. Therefore, we aim to reveal the mechanism of atorvastatin treatment for HCC by using network pharmacology and bioinformatics methods. The databases SwissTargetPrediction, PharmMapper, and DrugBank were utilized to obtain targets of atorvastatin, while GSE169289, GSE135631, and GSE207435 were used to identify differentially expressed genes (DEGs) for HCC. The overlap between the two groups was used to identify atorvastatin's target for treating HCC. Following protein-protein interaction (PPI) analysis, hub genes were identified using Cytoscape software and LASSO analysis. The hub genes were further validated using data from The Cancer Genome Atlas (TCGA) and The Human Protein Atlas (HPA) databases. To evaluate the clinical significance of the hub genes, Kaplan-Meier (KM) survival analysis and Cox analysis were conducted. Kyoto Encyclopedia of Genes and Genomes (KEGG) and Gene Set Enrichment Analysis (GSEA) were performed to investigate potential mechanisms. Finally, molecular docking analysis was performed to validate the interaction between atorvastatin and the hub genes. A total of 1948 DEGs of HCC and 380 targets of atorvastatin were identified, respectively. After taking the intersection, 79 genes were identified as potential targets of atorvastatin for HCC treatment. After multiple screening methods, CYP2C9 was ultimately identified as the hub gene. Analysis of data from TCGA and HPA databases showed reduced expression of CYP2C9 in HCC tissues. KM and Cox analysis showed a favorable prognosis for HCC patients with high CYP2C9 expression. KEGG and GSEA indicated that metabolism of xenobiotics by cytochrome P450, and PPAR signaling pathway could be the potential mechanisms for atorvastatin in treating HCC. Molecular docking analysis revealed that atorvastatin binds to CYP2C9 with a binding energy of - 8.837, indicating highly stable binding. CYP2C9 is associated with the prognosis of HCC patients and could serve as a potential target for atorvastatin treatment in HCC.

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阿托伐他汀治疗肝细胞癌的机制：基于网络药理学、分子对接和生物信息学分析的研究。

肝细胞癌（HCC）是一种发病率和死亡率都很高的肿瘤。目前的研究表明，他汀类药物可能有助于预防和治疗，但对相关机制的研究仍然有限。因此，我们旨在利用网络药理学和生物信息学方法揭示阿托伐他汀治疗 HCC 的机制。我们利用SwissTargetPrediction、PharmMapper和DrugBank数据库获得阿托伐他汀的靶点，并利用GSE169289、GSE135631和GSE207435鉴定HCC的差异表达基因（DEGs）。两组之间的重叠被用来确定阿托伐他汀治疗 HCC 的靶点。在进行蛋白-蛋白相互作用（PPI）分析后，利用Cytoscape软件和LASSO分析确定了中心基因。利用癌症基因组图谱（TCGA）和人类蛋白质图谱（HPA）数据库的数据进一步验证了中心基因。为了评估中心基因的临床意义，研究人员进行了Kaplan-Meier（KM）生存分析和Cox分析。为了研究潜在的机制，还进行了京都基因组百科全书（KEGG）和基因组富集分析（GSEA）。最后，进行了分子对接分析，以验证阿托伐他汀与枢纽基因之间的相互作用。结果发现，HCC 的 DEGs 共 1948 个，阿托伐他汀的靶点共 380 个。经过交叉分析，79 个基因被确定为阿托伐他汀治疗 HCC 的潜在靶点。经过多种筛选方法，最终确定 CYP2C9 为中心基因。对TCGA和HPA数据库数据的分析表明，CYP2C9在HCC组织中的表达减少。KM和Cox分析显示，CYP2C9高表达的HCC患者预后良好。KEGG和GSEA表明，细胞色素P450和PPAR信号通路对异种生物的代谢可能是阿托伐他汀治疗HCC的潜在机制。分子对接分析表明，阿托伐他汀与CYP2C9的结合能为-8.837，表明结合高度稳定。CYP2C9与HCC患者的预后有关，可作为阿托伐他汀治疗HCC的潜在靶点。

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来源期刊

Naunyn-Schmiedeberg's archives of pharmacology 医学-药学

CiteScore

6.20

自引率

5.60%

发文量

142

审稿时长

4-8 weeks

期刊介绍： Naunyn-Schmiedeberg''s Archives of Pharmacology was founded in 1873 by B. Naunyn, O. Schmiedeberg and E. Klebs as Archiv für experimentelle Pathologie und Pharmakologie, is the offical journal of the German Society of Experimental and Clinical Pharmacology and Toxicology (Deutsche Gesellschaft für experimentelle und klinische Pharmakologie und Toxikologie, DGPT) and the Sphingolipid Club. The journal publishes invited reviews, original articles, short communications and meeting reports and appears monthly. Naunyn-Schmiedeberg''s Archives of Pharmacology welcomes manuscripts for consideration of publication that report new and significant information on drug action and toxicity of chemical compounds. Thus, its scope covers all fields of experimental and clinical pharmacology as well as toxicology and includes studies in the fields of neuropharmacology and cardiovascular pharmacology as well as those describing drug actions at the cellular, biochemical and molecular levels. Moreover, submission of clinical trials with healthy volunteers or patients is encouraged. Short communications provide a means for rapid publication of significant findings of current interest that represent a conceptual advance in the field.