期刊文献+

TSA对食管癌细胞系EC9706细胞周期作用及分子机制的探讨 被引量:1

The molecular mechanism of TSA to esophagus cancer cell line EC9706 mitotic cycle function
下载PDF
导出
摘要 目的研究去乙酰化酶抑制剂曲古菌素A(TSA)对食管癌细胞EC9706细胞周期的作用及机制。方法将浓度为0.5、1.0、1.5μmol/L TSA作用EC9706细胞24 h,用MTT观察不同浓度TSA对EC9706细胞的生长抑制作用;流式细胞仪检测细胞生长及周期;Western Blot检测TSA对食管癌细胞周期相关基因的表达。结果 1.0μmol/L浓度的TSA对EC9706细胞有明显的生长抑制作用,并呈现一定的量效关系,在1.0μmol/L浓度之上可明显诱导食管癌细胞EC9706细胞周期阻滞,明显增强p21、p27基因的表达,明显降低CCND1、CDK4D基因的表达。结论一定剂量的TSA可抑制食管癌EC9706细胞的生长,通过调控多个细胞周期相关基因诱导食管癌细胞细胞周期阻滞,细胞阻滞的发生与p21、p27基因表达的增加及CCND1、CDK4D基因表达的减少相关。 Objective To study the deacetylase inhibitor TSA on the esophageal cancer cell EC9706 cell cycle effect and its mechanism.Methods 0.5,1.0,1.5 μmol/L TSA actin EC9706 cells 24 hours,the effects of different concentrations of TSA on EC9706 cell growth inhibition were observed by MTT,flow cytometry measured cell growth and cycle;TSA on esophageal cancer cell cycle-related genes expression by Western Blot test.Results 1.0 μmol/L concentration of TSA on the EC9706 inhibited the growth of cells and showed a definite dose-effect relationship,above 1.0 μmol/L concentration could significantly induce cell cycle arrest of esophageal cancer cell EC9706 could significantly enhance the p21,p27 gene expression,decreased CCND1,CDK4D gene expression.Conclusion The dose of TSA inhibite the growth of esophageal cancer EC9706 cells by regulating multiple cell cycle-related genes induced by esophageal cancer cells in cell cycle arrest,cell block occurrence revelant with p21,p27 gene expression increase and CCND1,CDK4D expression gene reduction.
出处 《重庆医学》 CAS CSCD 北大核心 2010年第20期2734-2736,共3页 Chongqing medicine
关键词 曲古菌素A 细胞周期 P21 P27 CCND1 CDK4D 食管癌细胞 trichostatin A mitotic cycle P21 P27 CCND1 CDK4D esophagus cancer cell
  • 相关文献

参考文献12

  • 1田凡清,陈新胜,谢军,胡菁.曲古菌素A对K562细胞中HDAC1表达的影响[J].中国现代医学杂志,2006,16(11):1642-1645. 被引量:5
  • 2And M,Hansen R,Ding RX,et a1.Disruption of 3D tissue integrity facilitates adenovirus infection by deregu lating the coxsackievirus and adenovirus receptor[J].Proc Natl Acad Sci USA,2003,100(4):1943.
  • 3Seoj S,Chon Y,Kim R,et al.Cell cycle arrest and lyticinduction of EBV-transformed B lymphoblastoid cells by a his-tone deacetylase inhibitor,Trichostatin A[J].Oncol Rep,2008,19(1):93.
  • 4张梅芳,云径平,苏曙光,张志毅,符珈,侯景辉,杨宇峰.原发性肝细胞癌组织中p53和p21^(WAF/CIP1)及MDM2蛋白的表达及其临床意义[J].中华肿瘤防治杂志,2007,14(15):1121-1124. 被引量:8
  • 5Radhakrishnan SK,Feficiano CS,Najmabadi F,et al.Constitutive expression of E2F-1 leads to p21-dependent cell cycle arrest in S phase of the cell cycle[J].Oncogene,2004,23(23):4173.
  • 6王振国,郭和清.膀胱癌Ha-ras基因突变、P^(21)蛋白表达及其意义[J].中国现代医学杂志,2003,13(8):59-60. 被引量:3
  • 7Kalpana S,Joshi.In vitro antitumor properties of a novel cyclin-dependent kinase inhibitor,P276-00[J].Mol Cancer Ther,2007,6(3):918.
  • 8Yu Q,Sicinska E,Geng Y,et al.Requirement for CDK4 kinase function in breast cancer[J].Cancer Cell,2006,9(1):23.
  • 9Henkens T,Papeleu P,Elautl G,et al.Trichostatin A,acritical factor in maintaining the functional differentiation of primary cultured rat hepatocytes[J].Toxicol Appl Pharmacol,2007,218(1):64.
  • 10Sachs MD,Rauen KA,Ramamurthy M,et al.Integrin V and coxsackie adenovirusreceptor expression in clinical bladder[J].Cancer Urology,2002,60:531.

二级参考文献17

共引文献11

同被引文献13

  • 1夏忠军,常建华,张力,姜文奇,管忠震,刘基巍,张阳,胡晓桦,吴国华,王华庆,陈正常,陈建超,周清华,陆建伟,樊青霞,黄建瑾,郑晓.基因工程腺病毒(H101)瘤内注射联合化疗治疗头颈部及食管鳞癌的Ⅲ期临床研究[J].癌症,2004,23(12):1666-1670. 被引量:50
  • 2孙淼淼,张红,曹学全,娄欣,高冬玲,张岚,宋一民,陈奎生.肝素酶特异性RNAi对人食管癌移植瘤组织中Hpa基因表达的影响[J].郑州大学学报(医学版),2007,42(1):12-14. 被引量:3
  • 3Wang Y,Hallden G,Hill R,et al.E3 gene manipulations affect oncolyric adenovirus activity in immunocompetent tumor models[J].Nat Biotechnol,2003,21 (11):1328-1335.
  • 4Wakayama M,Abei M,Kawashima R,et al.El A,El B double-restricted adenovirus with RGD-fiber modification exhibits enhanced oncolysis for CAR-deficient biliary cancers[J].Clin Cancer Res,2007,13(10):3043-3050.
  • 5Yamashita M,Ino A,Kawabata K,et al.Expression of coxsackie and adenovirus receptor reduces the lung metastatic potential of murine tumor cells[J].Int J Cancer,2007,121 (8):1690-1696.
  • 6Kitazono M,Goldsmith ME,Aikou T,et al.Enhanced adenovirus transgene expression in malignant cells treated with the histone deacetylase inhibitor FR901228[J].Cancer Res,2001,61 (17):6328-6330.
  • 7Honda T,Saitoh H,Masuko M,et al.The coxsackievirus-adenovirus receptor protein as a cell adhesion molecule in the developing mouse brain[J].Brain Res Mol Brain Res,2000,77(1):19-28.
  • 8Rauen KA,Sudilovsky D,Le JL,et al.Expression of the coxsackie adenovirus receptor in normal prostate and in primary and metastatic prostate carcinoma:potential relevance to gene therapy[J].Cancer Res,2002,62(13):3812-3818.
  • 9Okegawa T,Pong RC,Li Y,et al.The mechanism of the growth-inhibitory effect of coxsackie and adenovirus receptor (CAR) on human bladder cancer:a functional analysis of car protein structure[J].Cancer Res,2001,61 (17):6592-6600.
  • 10Fok PT,Huang KC,Holland PC,et al.The Coxsackie and adenovirus receptor binds microtubules and plays a role in cell migration[J].J Bid Chem,2007,282(10):7512-7521.

引证文献1

相关作者

内容加载中请稍等...

相关机构

内容加载中请稍等...

相关主题

内容加载中请稍等...

浏览历史

内容加载中请稍等...
;
使用帮助 返回顶部