基础医学与临床 ›› 2016, Vol. 36 ›› Issue (12): 1670-1674.

• 研究论文 • 上一篇    下一篇

顺铂诱导食管癌细胞系ECA109损伤机制

史鸿云,苑兰惠,杨会彬,苏雷,藤菲,周斌   

  1. 河北大学附属医院
  • 收稿日期:2016-04-21 修回日期:2016-09-26 出版日期:2016-12-05 发布日期:2016-11-29
  • 通讯作者: 史鸿云 E-mail:hyshi2012@sina.com
  • 基金资助:
    MCPH1蛋白表达调控体内外食管癌放疗敏感性研究;MCPH1蛋白表达调控体内外食管癌放疗敏感性研究

Mechanism of damage induced by cisplatin in esophageal cancer cell line ECA109

  • Received:2016-04-21 Revised:2016-09-26 Online:2016-12-05 Published:2016-11-29
  • Contact: Hong-yun SHI E-mail:hyshi2012@sina.com

摘要: 目的 探讨顺铂诱导食管癌细胞系ECA109 DNA 机制。方法 用MTT法测定ECA109细胞增殖,绘制细胞增殖曲线,筛选出低细胞毒性药物浓度用于后续实验。用免疫荧光法检测顺铂作用24 h 后50个ECA109细胞内r-H2AX、P-STAT1和CHK2-T68核内斑点(IF)平均数量。分别检测沉默H2AX基因和沉默STAT1基因前后,顺铂作用24 h后50个ECA109细胞内 r-H2AX、P-STAT1和CHK2-T68核内斑点(IF)平均数量。结果 顺铂呈时间剂量依赖性抑制ECA109细胞增殖。顺铂可以诱导ECA109细胞产生r-H2AX、P-STAT1和CHK2-T68核内斑点(IF)(P<0.05)。沉默H2AX基因使顺铂诱导的r-H2AX、P-STAT1和CHK2-T68核内斑点(IF)均减少(P<0.05)。沉默STAT1基因可以减少顺铂诱导的P-STAT1和CHK2-T68核内斑点(IF)生成(P<0.05)。结论 顺铂可以诱导食管癌细胞损伤,产生多种核内斑点(IF)。在这一损伤通路中,H2AX位于上游,调控STAT1和CHK2;STAT1位于H2AX下游,CHK2上游,可调控CHK2。

关键词: 食管癌, 顺铂, 损伤应答, 核内斑点

Abstract: Objective To investigate the mechanism of cisplatin-induced damage in the esophageal cancer cell line ECA109. Methods The proliferation with different time and concentrations of cisplatin was determined by MTT assay in ECA109 cells, the cell growth curve was drawn, and the low concentration drug,which be used in subsequent experiments,was selectd。The cisplatin induced nuclear foci (IF) average number changes of r-H2AX, P-STAT1 and CHK2-T68 at 24 h in 50 ECA109 cells were detected by immunofluorescence. The cisplatin induced nucleus foci (IF) average number changes of r-H2AX, P-STAT1 and CHK2-T68 at 24 h in 50 ECA109 cells were determined by immunofluorescence before and after silence H2AX gene or STAT1 respectively. Results The inhibition of proliferation induced by cisplatin in ECA109 cells were time and dose-dependent. Cisplatin can induce ECA109 cells to produce r-H2AX, P-STAT1 and CHK2-T68 nucleus foci (P<0.05). Cisplatin-induced r-H2AX, P-STAT1 and CHK2-T68 nucleus foci were reduced through silence H2AX gene, P<0.05. Cisplatin-induced P-STAT1 within CHK2-T68 nuclear foci were reduced by silence STAT1 gene (P<0.05). Conclusions Cisplatin can induce esophageal cancer cell injury, resulting in a variety of nuclear foci. In this damage response, H2AX is at the top regulating STAT1 and CHK2; STAT1 located downstream of H2AX and upstream of CHK2, adjusting CHK2.

Key words: Esophageal cancer, cisplatin, Damage response, Nuclear foci

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