[1]周定安,黄文芳,刘文,等.P53途径在辛伐他汀诱导K562细胞凋亡中的作用[J].陆军军医大学学报(原第三军医大学学报),2007,29(22):2160-2163.
 ZHOU Ding-an,HUANG Wen-fang,LIU Wen,et al.Role of P53 pathway in simvastatin-induced apoptosis of K562 cells in vitro[J].J Amry Med Univ (J Third Mil Med Univ),2007,29(22):2160-2163.
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P53途径在辛伐他汀诱导K562细胞凋亡中的作用(/HTML )
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陆军军医大学学报(原第三军医大学学报)[ISSN:1000-5404/CN:51-1095/R]

卷:
29卷
期数:
2007年第22期
页码:
2160-2163
栏目:
论著
出版日期:
2007-11-30

文章信息/Info

Title:
Role of P53 pathway in simvastatin-induced apoptosis of K562 cells in vitro
作者:
周定安黄文芳刘文胥国强杜琼赵慎许毅
重庆医科大学:附属儿童医院检验科,检验系,临床检验诊断学省部共建教育部重点实验室;四川省医学科学院四川省人民医院检验科;泸州医学院检验系
Author(s):
ZHOU Ding-an HUANG Wen-fang LIU Wen XU Guo-qiang DU Qiong ZHAO Shen XU Yi
Department of Clinical Laboratory, Children’s Hospital, Chongqing 400014, Department of Laboratory Medicine, Chongqing Medical University, Chongqing 400016;Clinical Laboratory Division, Sichuan People’s Hospital & Academy of Medical Sciences, Chengdu 610072; Laboratory Medicine Department, Luzhou Medical College, Luzhou 646000, China
关键词:
K562细胞P53通路凋亡
Keywords:
K562 cells P53 pathway apoptosis
分类号:
R73-361;R730.23;R733.72
文献标志码:
A
摘要:
目的  探讨辛伐他汀处理后的P53通路和细胞周期的分子水平变化,以说明P53途径在辛伐他汀抑制K562细胞增殖和诱导细胞凋亡中的作用。  方法  体外培养和用辛伐他汀处理K562细胞,用流式细胞仪检测辛伐他汀作用后的细胞周期和凋亡率的变化,用RT-PCR检测P53通路和细胞周期相关基因的变化。采用免疫组化LDP法检测P21蛋白变化的水平。  结果  辛伐他汀能使K562细胞停滞在G0/G1期,明显诱导K562细胞凋亡,大多数P53通路基因和细胞周期相关基因出现差异表达。P21蛋白随药物作用时间的延长,表达上调。  结论  P53通路可能在辛伐他汀诱导的K562细胞增殖抑制和凋亡发生的过程中起重要作用。
Abstract:
Objective    To investigate the changes of P53 pathway and cell cycle in K562 cells treated with simvastatin in molecular levels and illustrate the antiproliferative and apoptosis-induced role of P53 pathway in K562 cells when exposed to simvastatin.     Methods    K562 cells were cultured and treated with simvastatin in vitro. The apoptosis rate and cell cycle of K562 cells were measured by FCM. The transcriptional level changes of most molecules in P53 pathway and cell cycle were detected by RT-PCR. The changes of P21 protein was measured by immunohistochemistry LDP method.     Results    G0/G1 arrest in K562 cells and significant apoptosis of K562 cells were induced by simvastatin. Most genes in P53 pathway and genes related to cell cycle after exposed to simvastatin were expressed differentially in K562 cells. The P21 protein was up-regulated with the prolongation of simvastatin treatment time.     Conclusion    P53 pathway probably plays important roles in anti-proliferation and apoptosis of K562 cells induced by simvastatin.

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更新日期/Last Update: 2008-07-01