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WISp39基因对U937细胞增殖、凋亡和周期的影响
引用本文:李玥莹,刘黎琼,杨晶,刘伟,陈祥俊,李小青,杜雯,黄士昂. WISp39基因对U937细胞增殖、凋亡和周期的影响[J]. 中国实验血液学杂志, 2007, 15(4): 733-737
作者姓名:李玥莹  刘黎琼  杨晶  刘伟  陈祥俊  李小青  杜雯  黄士昂
作者单位:华中科技大学同济医学院附属协和医院干细胞研究中心,武汉,430022
摘    要:为了探讨一种新发现的p21调控蛋白WISp39对白血病细胞的增殖、凋亡和周期的影响,构建了WISp39的真核表达质粒pLenti6/V5-WISp39,并导入了人髓系白血病细胞系U937细胞,转染后用定量PCR检测了WISp39表达的变化,用CCK-8法测定细胞增殖活性,流式细胞术(FACS)检测细胞凋亡和周期的变化。结果显示:pLen-ti6/V5-WISp39转染48小时后,实验组中WISp39mRNA表达上升了(5.5±1.2)倍,同时U937细胞的增殖明显受到抑制,抑制率为37.6%;进一步的分析表明,在实验时间内,WISp39表达的升高不能明显诱导U937细胞的凋亡,但G0/G1期细胞比例由(40.59±0.7)%上升到(49.79±1.1)%。结论:WISp39对于U937无明显的诱导凋亡作用,但通过对细胞周期的影响,使停滞在G/G期的细胞增多,从而抑制了U937增殖。

关 键 词:U937细胞  细胞增殖  细胞周期
文章编号:1009-2137(2007)04-0733-05
修稿时间:2006-10-16

Effect of WISp39 on Proliferation, Cell Cycle and Apoptosis of U937 Cells
LI Yue-Ying,LIU Li-Qiong,YANG Jing,LIU Wei,CHEN Xiang-Jun,LI Xiao-Qing,DU Wen,HUANG Shi-Ang. Effect of WISp39 on Proliferation, Cell Cycle and Apoptosis of U937 Cells[J]. Journal of experimental hematology, 2007, 15(4): 733-737
Authors:LI Yue-Ying  LIU Li-Qiong  YANG Jing  LIU Wei  CHEN Xiang-Jun  LI Xiao-Qing  DU Wen  HUANG Shi-Ang
Affiliation:Center for Stem Cell Research and Application, Union Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan 430022, China
Abstract:To investigate the effect of a novel p21-modulating protein WISp39 on proliferation, apoptosis and cell cycle of leukemia cells, the plasmid pLenti6/V5-WISp39 was constructed and transfected into the human myelocytic leukemia cell line-U937 cells. The expression of WISp39 was detected by real-time PCR at 48 hours after transfection, proliferation of U937 cells assayed by CCK-8, apoptosis and cell cycle were determined by flow cytometry. The results showed that plasmid pLenti6/V5-WISp39 could readily enhance the expression of WISp39 in U937 cells. A significant growth inhibition (37.6%) was observed in cells tranfected with pLenti6/V5-WISp39, while the control plasmid pLenti6/V5-lacZ showed little effect on U937 growth. Further analysis revealed that pLenti6/V5-WISp39 did not show obvious apoptosis induction effect, but it could really regulate U937 proliferation via cell cycle modulation. Compared with pLenti6/V5-lacZ, pLenti6/V5-WISp39 resulted in increase of cells in G(0)/G(1) phase by 10% at 48 hours after transfection. It is concluded that the WISp39 gene has no significant apoptosis induction effect on leukemic cells, but it can increase cells at G(0)/G(1) phase via effect on cell cycle, thus inhibiting the U937 proliferation. This result means WISp39 gene can act as a negative modulator on tumour cells.
Keywords:WISp39  p21CIP1/WAF1
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