地榆皂苷Ⅱ通过ITGB4/FAK信号通路抑制非小细胞肺癌的进展OA
Ziyuglycoside Ⅱ Inhibit the Progression of Non-small Cell Lung Cancer through the ITGB4/FAK Signaling Pathway
背景与目的 非小细胞肺癌(non-small cell lung cancer,NSCLC)的发病率和死亡率总体呈现上升趋势,患者整体预后不佳,现有临床治疗手段存在明显的局限性.而中药生物活性成分具有作用靶点多样、毒副作用小的独特优势.地榆皂苷II(ziyuglycoside II,ZGS II)是地榆的一种主要活性成分,可抑制癌细胞的增殖、迁移以及侵袭过程,这一特性使其在癌症治疗领域展现出了潜在的应用价值和发展前景.然而,ZGS II对NSCLC的作用及其可能的机制仍未阐明.本研究旨在探讨ZGS II在NSCLC中抗肿瘤的分子机制,探讨作为改善NSCLC患者预后的一种新的治疗策略的可能性.方法 首先采用细胞增殖与毒性检测试剂盒(cell counting kit-8,CCK-8)和集落形成实验检测ZGS II处理NSCLC细胞后活力和增殖能力的变化.细胞划痕和Transwell实验评估ZGS II对NSCLC细胞的迁移和侵袭能力的影响.利用蛋白印迹法、慢病毒转染、细胞划痕和Transwell等方法研究ZGS II对整合素β4/黏着斑激酶(integrin β4/focal adhesion kinase,ITGB4/FAK)信号通路的作用.随后使用FAK激活剂ZINC40099027进行逆转实验.采用裸鼠异种移植模型评价ZGS II对体内NSCLC转移的抑制作用.结果 ZGS II抑制NSCLC细胞的增殖、迁移和侵袭,并且抑制了ITGB4的蛋白表达,这一结果在敲低ITGB4后抑制作用明显加强.同时发现总FAK的表达几乎不变,但磷酸化黏着斑激酶(phosphorylated focal adhesion kinase,p-FAK)的蛋白表达水平受到抑制.加入FAK激活剂后,细胞的迁移率以及穿过Transwell膜的细胞数量增加,ZGS II对细胞迁移和侵袭能力的抑制作用得到逆转.因此,ZGS II的抗肿瘤作用依赖于ITGB4/FAK信号通路的激活减弱.裸鼠异种移植实验结果表明,ZGS II显著抑制了裸鼠体内肿瘤的生长.结论 ZGS II通过抑制ITGB4/FAK通路抑制NSCLC的增殖、转移和肿瘤生长.这些结果突出了ZGS II作为治疗转移性NSCLC的药物的前景,为其临床研究奠定基础.
Background and objective The incidence and mortality rates of non-small cell lung cancer(NSCLC)are generally on the rise,and the overall prognosis of patients remains poor.Current clinical treatment strategies have signifi-cant limitations.Notably,the bioactive components of traditional Chinese medicine possess unique advantages,including diverse targets of action and low toxicity.Ziyuglycoside II(ZGS II),a major active component of Sanguisorba officinalis L,has been shown to inhibit cancer cell proliferation,migration,and invasion.This property confers potential application value and developmental prospects for its use in cancer therapy.Nevertheless,the effects of ZGS II on NSCLC and the underlying mechanisms remain unclear.This study aimed to investigate the anti-tumor molecular mechanism of ZGS II in NSCLC and to explore the potential of being a novel therapeutic strategy for improving the prognosis of NSCLC patients.Methods First,the cell counting kit-8(CCK-8)and the colony formation assay were used to detect the changes in the viability and prolifera-tion ability of NSCLC cells after treatment with ZGS II.Wound-healing and Transwell assays were used to evaluate the effects of ZGS II on migration and invasion abilities.Western blot,Lentiviral transfection,wound healing assay,and Transwell assay were used to study the effects of ZGS II on the integrin β4/focal adhesion kinase(ITGB4/FAK)signaling pathway.A rescue experiment was then performed using the FAK agonist ZINC40099027.A nude mouse xenograftmodel was used to evaluate the inhibitory effect of ZGS II on NSCLC metastasis in vivo.Results ZGS II inhibited proliferation,migration,and invasion of NSCLC cells and suppressed the protein expression of ITGB4.This inhibitory effect was significantly enhanced upon ITGB4 knockdown.Meanwhile,total FAK expression remained nearly unchanged,but the protein expression level of phosphorylated focal adhesion kinase(p-FAK)was suppressed.Following the addition of an FAK activator,cell migration rate and the number of cells crossing the Transwell membrane increased,reversing the inhibitory effects of ZGS II on cell migration and invasion.Therefore,the anti-tumor effect of ZGS II depends on the reduced activation of the ITGB4/FAK signaling pathway.The nude mouse xenograftexperiment results showed that ZGS II effectively inhibited tumor growth in nude mice.Conclusion ZGS II inhibits proliferation,metastasis,and tumor growth in NSCLC by suppressing the ITGB4/FAK pathway.These findings high-light the potential of ZGS II as a promising drug for treating metastatic NSCLC and lay the foundation for its clinical research.
任佳旋;刘雅妮;王博;吕嘉益;邸韫博;陈振文;徐义荣
030000 太原,山西医科大学研究生学院||032200 汾阳,山西医药学院基础医学部030000 太原,山西医科大学研究生学院||032200 汾阳,山西医药学院基础医学部030000 太原,山西医科大学研究生学院||032200 汾阳,山西医药学院基础医学部030000 太原,山西医科大学研究生学院||032200 汾阳,山西医药学院基础医学部030000 太原,山西医科大学研究生学院||032200 汾阳,山西医药学院基础医学部030000 太原,山西医科大学研究生学院030000 太原,山西医科大学研究生学院||032200 汾阳,山西医药学院基础医学部||032200 汾阳,山西省汾阳医院病理科
肺肿瘤地榆皂苷ⅡITGB4/FAK信号通路进展
Lung neoplasmsZiyuglycoside ⅡITGB4/FAK pathwayProgression
《中国肺癌杂志》 2026 (4)
251-262,12
本研究受山西省卫生健康委员会人才项目(No.2024224)和吕梁市分子病理重点实验室项目(No.ZDSYS06)资助 This study was supported by the grants from Talent Project of Shanxi Provincial Health Commission(No.2024224,to Yirong XU)and Key Laboratory of Molecular Pathology in Lvliang City(No.ZDSYS06,to Yirong XU).
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