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首页> 美国卫生研究院文献>Molecular Cellular Proteomics : MCP >Proteomic Analysis Revealed the Important Role of Vimentin in Human Cervical Carcinoma HeLa Cells Treated With Gambogic Acid
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Proteomic Analysis Revealed the Important Role of Vimentin in Human Cervical Carcinoma HeLa Cells Treated With Gambogic Acid

机译:蛋白质组学分析揭示波形蛋白在用藤黄酸治疗的宫颈癌HeLa细胞中的重要作用

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Gambogic acid (GA) is an anticancer agent in phase IIb clinical trial in China. In HeLa cells, GA inhibited cell proliferation, induced cell cycle arrest at G2/M phase and apoptosis, as showed by results of MTT assay and flow cytometric analysis. Possible target-related proteins of GA were searched using comparative proteomic analysis (2-DE) and nine proteins at early (3 h) stage together with nine proteins at late (24 h) stage were found. Vimentin was the only target-related protein found at both early and late stage. Results of both 2-DE analysis and Western blotting assay suggested cleavage of vimentin induced by GA. MS/MS analysis of cleaved vimentin peptides indicated possible cleavage sites of vimentin at or near ser51 and glu425. Results of targeted proteomic analysis showed that GA induced change in phosphorylation state of the vimentin head domain (aa51–64). Caspase inhibitors could not abrogate GA-induced cleavage of vimentin. Over-expression of vimentin ameliorated cytotoxicity of GA in HeLa cells. The GA-activated signal transduction, from p38 MAPK, heat shock protein 27 (HSP27), vimentin, dysfunction of cytoskeleton, to cell death, was predicted and then confirmed. Results of animal study showed that GA treatment inhibited tumor growth in HeLa tumor-bearing mice and cleavage of vimentin could be observed in tumor xenografts of GA-treated animals. Results of immunohistochemical staining also showed down-regulated vimentin level in tumor xenografts of GA-treated animals. Furthermore, compared with cytotoxicity of GA in HeLa cells, cytotoxicity of GA in MCF-7 cells with low level of vimentin was weaker whereas cytotoxicity of GA in MG-63 cells with high level of vimentin was stronger. These results indicated the important role of vimentin in the cytotoxicity of GA. The effects of GA on vimentin and other epithelial-to-mesenchymal transition (EMT) markers provided suggestion for better usage of GA in clinic.
机译:藤黄酸(GA)是在中国IIb期临床试验中使用的抗癌药。 MTT分析和流式细胞仪分析结果表明,GA可抑制HeLa细胞的增殖,诱导其在G2 / M期的细胞周期停滞以及凋亡。使用比较蛋白质组分析(2-DE)搜索可能的GA靶标相关蛋白,发现早期(3 h)的9种蛋白质以及晚期(24 h)的9种蛋白质。波形蛋白是在早期和晚期均发现的唯一靶标相关蛋白。 2-DE分析和Western印迹分析的结果表明GA诱导的波形蛋白裂解。切割的波形蛋白肽的MS / MS分析表明,波形蛋白可能在ser51和glu425或附近断裂。靶向蛋白质组学分析的结果表明,GA诱导波形蛋白头部结构域(aa51–64)的磷酸化状态发生变化。半胱天冬酶抑制剂不能消除GA诱导的波形蛋白的切割。波形蛋白的过度表达改善了HeLa细胞中GA的细胞毒性。从p38 MAPK,热休克蛋白27(HSP27),波形蛋白,细胞骨架功能障碍到细胞死亡的GA激活信号转导被预测,然后被证实。动物研究结果表明,GA处理可抑制HeLa荷瘤小鼠的肿瘤生长,在GA处理的动物的异种移植物中可观察到波形蛋白的切割。免疫组织化学染色的结果还显示,GA处理动物的异种移植物中波形蛋白水平下调。此外,与GA对HeLa细胞的细胞毒性相比,波形蛋白水平低的MCF-7细胞中GA的细胞毒性更弱,而波形蛋白水平较高的MG-63细胞中GA的细胞毒性更强。这些结果表明波形蛋白在GA的细胞毒性中的重要作用。 GA对波形蛋白和其他上皮-间质转化(EMT)标记的影响为临床更好地使用GA提供了建议。

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