The Mechanism of Scopolamine’s Effect on Migration Function of Lung Cancer Cells: A Network Pharmacology and Bioinformatics Perspective

IF 2.2 4区 医学 Q2 MEDICINE, GENERAL & INTERNAL
Yang Xiao, Mengcong Ma, Qing Gu, Yunfeng Xiao
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引用次数: 0

Abstract

Background. This study utilized network pharmacology and bioinformatics analysis to identify the hub genes influenced by scopolamine in lung cancer. Methods. The effect of scopolamine on lung cancer was investigated by cell invasion assay and cell scratch assay. The analysis involved protein-protein interaction (PPI) networks topology analysis to identify these genes, and subsequent differential analysis and survival analysis were conducted using gene expression profile interaction analysis (GEPIA). Furthermore, the findings were supported by molecular docking experiments for verification. Results. Results from cell invasion and scratch assays suggest that scopolamine inhibits the migration of lung cancer cells. JAK2, JAK3, CCR5, and ACE were identified as the top four hub genes that have an impact on lung cancer. KEGG enrichment analysis revealed that the scopolamine response in lung cancer is significantly associated with ten pathways, including “neuroactive ligand-receptor interaction in cancer,” “PD-1 checkpoint pathway in cancer,” “chemokine signaling pathway,” “PD-L1 expression,” and others. Additionally, the expression levels of JAK2, JAK3, CCR5, and ACE were found to be correlated with survival in patients with lung cancer. Furthermore, molecular docking experiments demonstrated that scopolamine binds and forms stable complexes with the protein products of all four aforementioned genes. The main targets of scopolamine in the treatment of lung cancer are JAK2, JAK3, CCR5, and ACE. Conclusion. Scopolamine has a significant effect on various cellular functions in lung cancer cells, potentially reducing the likelihood of metastasis. Based on these findings, it is recommended to consider administering scopolamine as part of the preoperative phase for patients with lung cancer.

Abstract Image

东莨菪碱影响肺癌细胞迁移功能的机制:网络药理学和生物信息学视角
研究背景本研究利用网络药理学和生物信息学分析来确定东莨菪碱对肺癌影响的枢纽基因。方法通过细胞侵袭试验和细胞划痕试验研究东莨菪碱对肺癌的影响。分析包括蛋白质-蛋白质相互作用(PPI)网络拓扑分析,以确定这些基因,随后使用基因表达谱相互作用分析(GEPIA)进行差异分析和生存分析。此外,研究结果还得到了分子对接实验的验证。结果细胞侵袭和划痕实验结果表明,东莨菪碱能抑制肺癌细胞的迁移。JAK2、JAK3、CCR5和ACE被确定为对肺癌有影响的前四个枢纽基因。KEGG富集分析显示,东莨菪碱在肺癌中的反应与 "癌症中的神经活性配体-受体相互作用"、"癌症中的PD-1检查点通路"、"趋化因子信号通路"、"PD-L1表达 "等十条通路显著相关。此外,研究还发现 JAK2、JAK3、CCR5 和 ACE 的表达水平与肺癌患者的生存率相关。此外,分子对接实验表明,东莨菪碱能与上述所有四种基因的蛋白产物结合并形成稳定的复合物。东莨菪碱治疗肺癌的主要靶点是JAK2、JAK3、CCR5和ACE。结论东莨菪碱对肺癌细胞的各种细胞功能有明显影响,有可能降低转移的可能性。基于这些发现,建议考虑在肺癌患者术前阶段使用东莨菪碱。
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来源期刊
CiteScore
5.30
自引率
0.00%
发文量
274
审稿时长
3-8 weeks
期刊介绍: IJCP is a general medical journal. IJCP gives special priority to work that has international appeal. IJCP publishes: Editorials. IJCP Editorials are commissioned. [Peer reviewed at the editor''s discretion] Perspectives. Most IJCP Perspectives are commissioned. Example. [Peer reviewed at the editor''s discretion] Study design and interpretation. Example. [Always peer reviewed] Original data from clinical investigations. In particular: Primary research papers from RCTs, observational studies, epidemiological studies; pre-specified sub-analyses; pooled analyses. [Always peer reviewed] Meta-analyses. [Always peer reviewed] Systematic reviews. From October 2009, special priority will be given to systematic reviews. [Always peer reviewed] Non-systematic/narrative reviews. From October 2009, reviews that are not systematic will be considered only if they include a discrete Methods section that must explicitly describe the authors'' approach. Special priority will, however, be given to systematic reviews. [Always peer reviewed] ''How to…'' papers. Example. [Always peer reviewed] Consensus statements. [Always peer reviewed] Short reports. [Always peer reviewed] Letters. [Peer reviewed at the editor''s discretion] International scope IJCP publishes work from investigators globally. Around 30% of IJCP articles list an author from the UK. Around 30% of IJCP articles list an author from the USA or Canada. Around 45% of IJCP articles list an author from a European country that is not the UK. Around 15% of articles published in IJCP list an author from a country in the Asia-Pacific region.
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