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甲胎蛋白激活PI3K/AKT信号促使肝癌Bel 7402细胞抗全反式维甲酸诱导凋亡 被引量:4

The anti-apoptotic effect of cytoplasmic alpha-fetoprotein in hepatoma cells induced by all-trans retinoic acid involves activation of the PI3K/AKT signaling pathway
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摘要 目的 研究甲胎蛋白(AFP)对肝癌细胞内PI3K/AKT信号传递的影响,以及其在癌细胞耐受全反式维甲酸(ATRA)中的作用. 方法 四甲基偶氮唑盐(MTT)法检测ATRA对人肝癌Bel 7402细胞增殖的影响;显微照相观察细胞形态学的改变;流式细胞分析细胞凋亡;激光共聚焦显微镜观察AFP与PTEN的共定位;免疫共沉淀(Co-IP)技术研究AFP与PTEN相互作用;Westemblot法分析磷酸化的蛋白激酶B(pAKT)和Src表达,构建干扰AFP表达的载体(AFP-siRNA)并转染Bel 7402细胞;用PI3K特异性阻断剂Ly294002处理细胞,分析Ly294002的作用效果.通过t检验分析组间的统计学差异. 结果 MTT分析显示,人肝癌Bel 7402耐受ATRA的细胞毒性;共聚焦显微镜观察显示AFP与PTEN共定位于细胞质;Co-IP技术研究发现AFP能与PTEN结合;MTT分析发现,Bel 7402细胞转染AFP-siRNA载体后24 h后,细胞生长显著受抑制,与对照组比较,差异有统计学意义(P<0.05),而且AFP-siRNA载体和ATRA共同处理组,细胞生长受到抑制更为显著,与对照组、单独处理组比较,差异均有统计学意义(P< 0.01);干扰AFP表达能显著增加Bel 7402细胞对ATRA敏感性,并能抑制pAKT和Src的表达;Ly294002能抑制AFP促进Bel 7402细胞表达pAKT和Src的作用.结论 肝癌细胞内表达的AFP能与PTEN结合并抑制PTEN对AKT的去磷酸化作用,肝癌细胞内高表达的AFP能激活PI3K/AKT信息通路对抗ATRA诱导的凋亡. Objective To explore the effect ofalpha-fetoprotein (AFP) on transduction of the PI3K/ AKT signal in hepatocellular carcinoma cells and the role played by AFP in resistance to cytotoxicity of all-trans retinoic acid (ATRA).Methods The effects of ATRA of human liver cancer cells was assessed using the BEL-7402 cell line with the MTT assay (to evaluate proliferation),microscopy (to evaluate morphology),flow cytometry (to evaluate apoptosis),laser confocal microscopy and coimmunoprecipitation (co-IP; to evaluate co-localization and interaction of AFP with PTEN),Western blotting (to evaluate expression of phosphorylated-protein kinase B (pAKT) and Src,and RNA interference (RNAi)-mediated knockdown of AFP.Finally,applicationof the PI3K-specific inhibitor Ly294002 was used to monitor the influence of AFP in transduction of the PI3K signal pathway.Results The human hepatoma cell line BEL-7402 were resistant to ATRA cytotoxicity.PTEN and AFP co-localized in the cytoplasm,and co-IP indicated that AFP interacts with PTEN in BEL-7402 cells.RNAi knockdown of AFP expression led to reduced growth of BEL-7402 cells.BEL-7402 cells transfected with AFP-short interfering (si)RNA vectors showed enhanced sensitivity to ATRA and reduced expression of pAKT(Ser473) and Src; Ly294002 reduced the role of AFP in stimulating expression ofpAKT(Ser473) and Src.Conclusion AFP can activate transduction of the PI3K/AKT signal,and expression of AFP in hepatoma cells is a pivotal event for resisting ATRA-induced apoptosis.
作者 朱明月 郭峻莉 夏华 李伟 鲁琰 董栩 陈栘 符史干 谢协驹 李孟森
机构地区 海南医学院海南省肿瘤发生和干预重点实验室 海南医学院分子生物重点实验室 海南医学院病理生理学教研室 海南医学院肿瘤研究所 广西医科大学研究生学院
出处 《中华肝脏病杂志》 CAS CSCD 北大核心 2014年第11期837-842,共6页 Chinese Journal of Hepatology
基金 国家自然科学基金(81360307,81260306,81160261,31060164,30960153) 教育部新世纪优秀人才支持计划(NCET-10-0124),教育部科技重点项目(211146)l海南省科技重点项目(DZXM20110038) 海南省自然科学基金(309034,310044,811208)
关键词 肝细胞 甲胎蛋白 耐药 PI3K/AKT信号通路 全反式维甲酸 Carcinoma,hepatocellular Alpha-fetoprotein Drug resistance PI3K/AKT signal pathway
分类号 R735.7 [医药卫生—肿瘤]
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参考文献21

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二级参考文献19

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共引文献10

同被引文献41

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中华肝脏病杂志
2014年 第11期

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