白术内酯III通过抑制成纤维细胞生长因子受体1、2和-4的表达增强多西紫杉醇对胃癌细胞的抗肿瘤作用

Yanxia Ji, Zhenqiao Kang, Ning Kang, Yanzheng Zhao, Q. Guo, Yongge Chen
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引用次数: 9

摘要

背景:据报道,天然活性成分在癌症治疗的临床实践中可作为辅助药物。然而,白术内酯III (ATL)的抗肿瘤作用很少被报道。在本研究中,我们评估了ATL联合多西紫杉醇对胃癌细胞的作用。方法采用CCK-8细胞毒法和ldh细胞毒法分别评价细胞活力和细胞毒活性。western blotting检测蛋白表达水平。Annexin V-FITC/PI染色采用流式细胞术检测细胞凋亡情况。结果ATL联合多西紫杉醇组ags和SGC-7901细胞活力明显低于单药组。联合治疗组LDH水平、细胞凋亡率、BAX / Bcl-2比值均明显高于单独治疗组。有趣的是,与单独多西紫杉醇治疗相比,多西紫杉醇联合ATL导致FGFR1、FGFR2和FGFR4蛋白表达显著降低。在AGS和SGC-7901细胞中,敲除FGFR1、-2和-4表现出与药物抑制生长和诱导凋亡相似的作用。结论satl和多西紫杉醇在抑制胃癌细胞生长和诱导凋亡方面具有协同作用,其潜在机制至少部分是通过抑制FGFR1、-2和-4介导的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Atractylenolide III Enhances the Anti-Neoplastic Efficacy of Docetaxel in Gastric Cancer Cell by Inhibiting Fibroblast Growth Factor Receptors 1, -2, and -4 Expression.
BACKGROUND Natural active components have been reported to serve as adjuvant medications in the clinical practice of cancer therapeutics. However, the antineoplastic roles of atractylenolide III (ATL) are rarely reported. In the present study, we assessed the functions of ATL combined with docetaxel in gastric cancer cells. METHODS Cell viability and cytotoxic activity were evaluated using CCK-8 and LDH-based cytotoxicity assays, respectively. Protein expression levels were measured by western blotting analysis. Annexin V-FITC/PI staining was used to evaluate cell apoptosis using flow cytometry. RESULTS AGS and SGC-7901 cell viability was significantly inhibited in ATL combined with docetaxel group compared with docetaxel treatment alone. The levels of LDH, apoptosis rate, and the ratio of BAX to Bcl-2 were significantly elevated in combination treatment group compared to docetaxel treatment alone. Intriguingly, docetaxel combined with ATL resulted in a significant decrease in FGFR1, FGFR2, and FGFR4 protein expression compared with docetaxel treatment alone. Knockout of FGFR1, -2, and -4 exhibited a similar role of medications to inhibit growth and induce apoptosis in AGS and SGC-7901 cells. CONCLUSIONS ATL and docetaxel treatment performed the synergistic effects on the inhibition of growth and induction of apoptosis in gastric cancer cells, and the underlying mechanism was mediated, at least partially, through the inhibition of FGFR1, -2, and -4.
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