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GSK525762A对KU812细胞增殖与凋亡的影响及其作用机制 被引量:1

Effect of BRD4 Inhibitor GSK525762A on Proliferation and Apoptosis of KU812 Leukemic Cells and Its Mechanism
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摘要 本研究旨在观察4型含Bromo结构域蛋白(bromodomain-containing protein 4,BRD4)抑制剂GSK52-5762A对KU812细胞增殖及凋亡的影响及其机制。用GSK525762A 100、250、500、1000、2500和5000 nmol/L处理KU812细胞48和72 h,CCK-8法检测其对细胞增殖的影响;GSK525762A 1.0、2.5和5.0μmol/L处理72 h,利用流式细胞术检测其对KU812细胞的凋亡诱导作用。将KU812细胞经DMSO和2.5μmol/L的GSK525762A处理后,利用实时荧光定量PCR观察c-Myc、BCL-2、CDK6、BCL-xL、BAK和BAX基因的mRNA表达水平。结果表明,GSK525762A能显著抑制KU812细胞的增殖,且抑制作用存在量-效关系(r=0.970)和时-效关系(r=0.956);GSK525762A能促进KU812细胞的凋亡;GSK525762A处理后促增殖基因c-Myc、CDK6和抗凋亡基因BCL-2和BCL-xL的mRNA较对照组降低,而促凋亡基因BAK和BAX的转录水平较对照组升高。结论:GSK525762A显著抑制KU812细胞的增殖并促进其凋亡,其机制可能与下调c-Myc、BCL-2、CDK6、BCL-xL的表达和上调BAK、BAX的表达有关。 This study was purposed to investigate the effect of bromodomain-containing protein 4 (BRD4) inhibitor GSK525762A on the proliferation and apoptosis of chronic myeloid leukemia blast crisis KU812 cells and its mechanism.KU812 cells were treated with different concentrations of GSK525762A (100,250,500,1 000,2 500 and 5000 nmol/L) and the inhibitory effects of drug on KU812 cell proliferation after 48 and 72 hours were detected by using CCK-8 assay.KU812 cells were treated with 3 different concentrations of GSK525762A (1.0,2.5 and 5 μmoL/L) and the cell apoptosis after 72 hours were assayed by using flow cytometry.KU812 cells were treated with DMSO and 2.5 μmol/L GSK525762A,and the mRNA levels of C-MYC,BCL-2,CDK6,BCL-xL,BAK and BAX were determined by using quantitative reverse transcription polymerase chain reaction (qRT-PCR).The results showed that GSK525762A could significantly inhibit the proliferation of KU812 cells and the inhibitory effect on KU812 cell proliferation was dependent on the dose-course and time-course of GSK525762A treatment.GSK525762A treatment could induce apoptosis of KU812 cells in a dose-dependent manner.After GSK525762A treatment,the mRNA levels of proliferation-promoting genes (C-MYC and CDK6) and pro-survival genes (BCL-2 and BCL-xL) decreased,while the transcription level of proapoptosis genes BAK and BAX increased,as compared to that of the control group.It is concluded that GSK525762A can inhibit the proliferation of KU812 cells and induce cell apoptosis possibly through depressing the transcription of CMYC,BCL-2,CDK6 and BCL-xL gene,and down-regulating BAK and BAX transcription.
作者 徐杰 王力 宋旭光 吴庆运 赵恺 曾令宇 韩正祥 陈翀 徐开林
机构地区 徐州医学院附属医院血液科 徐州医学院附属医院肿瘤科
出处 《中国实验血液学杂志》 CAS CSCD 北大核心 2014年第5期1239-1244,共6页 Journal of Experimental Hematology
基金 国家自然科学基金项目(81200210)
关键词 4型含Bromo结构域蛋白 GSK525762A KU812细胞 慢性粒细胞白血病急变 bromodomain-containing protein 4 GSK525762A KU812 cell CML blast crisis
分类号 R733.72 [医药卫生—肿瘤]
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参考文献11

  • 1Cortes JE,Talpaz M,Kantarjian H.Chronic myelogenous leukemia:a review.Am J Med,1996;100(5):555-570.
  • 2Zeng L,Zhou MM.Bromodomain:an acetyl-lysine binding domain.FEBS Lett,2002;513(1):124-128.
  • 3Dey A,Chitsaz F,Abbasi A,et al.The double bromodomain protein Brd4 binds to acetylated chromatin during interphase and mitosis.Proc Natl Acad Sci USA,2003;100(15):8758-8763.
  • 4Fielding AK.Current treatment of Philadelphia chromosome-positive acute lymphoblastic leukemia.Hematology Am Soc Hematol Educ Program,2011;2011:231-237.
  • 5Maruyama T,Farina A,Dey A,et al.A Mammalian bromodomain protein,brd4,interacts with replication factor C and inhibits progression to S phase.Mol Cell Biol,2002;22(18):6509-6520.
  • 6Jang MK,Mochizuki K,Zhou M,et al.The bromodomain protein Brd4 is a positive regulatory component of P-TEFb and stimulates RNA polymerase II-dependent transcription.Mol Cell,2005;19(4):523-534.
  • 7Poloni A,Serrani F,Berardinelli E,et al.Telomere length,c-myc and mad-1 expression could represent prognosis markers of myelodysplastic syndrome.Leuk Res,2013;37(11):1538-1544.
  • 8Cory S,Huang DC,Adams JM.The Bcl-2 family:roles in cell survival and oncogenesis.Oncogene,2003;22(53):8590-8607.
  • 9刘海波,张梅,李呈亮,贺鹏程.氯法拉滨对NB4细胞的增殖抑制作用及对Bcl-2表达的影响[J].中国实验血液学杂志,2012,20(3):571-573. 被引量:3
  • 10Zuber J,Shi J,Wang E,et al.RNAi screen identifies Brd4 as a therapeutic target in acute myeloid leukaemia.Nature,2011;478(7370):524-528.

二级参考文献10

  • 1Jeha S, Kantariian H. Clofarabine for the treatment of acute lymphoblastic leukemia. Expert Rev Anticancer Ther,2007 ;7 (2) : 113 -118.
  • 2Hannun YA. Apoptosis and the dilemma of cancer chemotherapy. Blood, 1997;89(6):1845-1853.
  • 3McDonald LR, McCarthy CH. Nursing considerations for clofarabine in the treatment of acute lymphoblastic leukemia in children. Clin J Oncol Nurs, 2006;10(6) :809 -815.
  • 4Pattingre S, Tassa A, Qu XP, et al. Bcl-2 antiapoptosis proteins inhibit Beclin 1 -dependent autophagy. Cell, 2005 ; 122 ( 6 ) : 927 - 939.
  • 5Atkinson EA, Barry M, Darmon AJ, et al. Cytotoxic T lymphocyte-assisted suicide. Caspase 3 activation is primarily the result of the direct action of granzyme B. J Biol Chem, 1998;273 (33) :21261 -21266.
  • 6Boise LH, Thompson CB. Bcl-x (L) can inhibit apoptosis in cells that have undergone Fas-induced protease activation. Proc Natl Acad Sci USA, 1997 ;94 (8) :3759 - 3764.
  • 7Saelens X, Festjens N, Vande Walle L, et al. Toxic proteins released from mitochondria in cell death. Oncogene,2004 ;23 ( 16 ) : 2861 - 2874.
  • 8Steganis L. Caspase-dependent and independent neuronal death:two distinct pathways to neuronal injury. Neuroscientist, 2005 ; 1 I ( 1 ) : 50 -62.
  • 9Hirsch T, Dallaporta B, Zamzami N, et al. Proteasome activation occurs at an early, premitochondrial step of thymocyte apoptosis. Immunology, 1998 ; 161 ( 1 ) : 35 -40.
  • 10Boatright KM, Salvesen GS. Mechanisms of caspase activation. Curr Opin Cell Biol, 2003; 15(6) :725 -731.

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中国实验血液学杂志
2014年 第5期

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