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铁剥夺和铁超负荷对白血病细胞株HL-60凋亡的影响机制
引用本文:王叨,李四保,刘玉峰.铁剥夺和铁超负荷对白血病细胞株HL-60凋亡的影响机制[J].中国小儿血液与肿瘤杂志,2012,17(3):110-112.
作者姓名:王叨  李四保  刘玉峰
作者单位:1. 450052,郑州大学第一附属医院儿内科
2. 450052,郑州大学第三附属医院儿内科
摘    要:目的探讨铁剥夺和铁超负荷对白血病细胞株HL-60细胞凋亡的影响及其机制,为临床采用铁剥夺策略治疗或辅助治疗白血病提供理论依据。方法在HL-60细胞培养基中分别加入不同浓度的去铁胺(DFO)或三氯化铁(FeCl3),造成细胞内铁剥夺或铁超负荷状态,采取噻唑蓝(MTT)法、DNA原位末端标记染色法(TUNEL)、免疫组化法检测铁剥夺和铁超负荷状态下HL-60细胞活力、凋亡率、细胞色素C(Cyt C)阳性细胞率。结果 DFO组细胞活力呈明显下降趋势,凋亡率呈显著上升趋势;FeCl3组细胞活力和凋亡率与对照组相比呈下降趋势;DFO组细胞胞浆内Cyt C阳性细胞率与对照组相比明显升高;而FeCl3组细胞浆内Cyt C阳性细胞率与对照组相比无明显差异。结论铁剥夺可促进线粒体释放Cyt C,诱导HL-60细胞凋亡;铁超负荷对线粒体释放Cyt C无直接影响作用。

关 键 词:铁剥夺  铁超负荷  细胞凋亡  细胞色素C

The influence of iron deprivation and rich iron on the apoptosis of human Leukemia-60 cells
WANG Dao , LI Sibao , LIU Yufeng.The influence of iron deprivation and rich iron on the apoptosis of human Leukemia-60 cells[J].Journal of China Pediatric Blood and Cancer,2012,17(3):110-112.
Authors:WANG Dao  LI Sibao  LIU Yufeng
Institution:2,LIU Yufeng1.1Department of Pediatrics,the First Affiliated Hospital of Zhengzhou University;2Department of Pediatrics,the Third Affiliated Hospital of Zhengzhou University,Zhengzhou 450052,China
Abstract:Objective To explore the influence and mechanism of iron deprivation and rich iron on the apoptotic process of human Leukemia-60(HL-60) cells,and provide the theoretical basis for the clinical therapy.Methods HL-60 cells were cultivated with different concentration of DFO and FeCl3 to establish intracellular iron-deprivated and rich-iron states.Cell viability,apoptotic rate and the positive rate of Cyt C were detected by MTT,TUNEL and immunohistochemistry.Results The cell viability in DFO-treated group decreased,while the apoptotic rate increased dramatically.In contrast,an opposite result was obtained in FeCl3-treated group.The positive rate of Cyt C in DFO-treated group was elevated,but no difference was found in FeCl3-treated group.Conclusions Iron deprivation induces apoptosis of HL-60 cells by releasing Cyt C from mitochondria,while rich iron has no direct impact on it.The mechanism of HL-60 cell proliferation might be related with the apoptosis-related genes in the upstream of the mitochondrial pathway.
Keywords:Iron deprivation  Iron overload  Human leukemia-60 cell  Apoptosis  Cytochrome C
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