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目的研究亚砷酸钠和三氧化二砷对人正常肝细胞L02增殖与凋亡效应的影响。方法分别采用亚砷酸钠和三氧化二砷处理人正常肝细胞L02,比色实验和集落形成实验检测细胞存活率,流式细胞术检测细胞凋亡和细胞周期分布,试剂盒法测定细胞内活性氧水平和谷胱甘肽含量,微核实验评价细胞染色体损伤。结果随着亚砷酸钠或三氧化二砷染毒浓度的增加,L02细胞的存活率、集落形成率和谷胱甘肽含量均下降,而集落形成抑制率、凋亡率、活性氧水平和微核率均增加,此外细胞周期都被阻滞在G2/M期。结论亚砷酸钠和三氧化二砷均能诱导人正常肝细胞L02活性氧增加和谷胱甘肽含量下降,继而引起细胞染色体损伤、细胞凋亡、细胞周期阻滞和细胞生长抑制,提示氧化应激是亚砷酸钠和三氧化二砷"致癌"与"治癌"共同的分子机制。
Abstract:Objective To explore the proliferation and apoptosis effects induced by sodium arsenite and arsenic trioxide on human hepatocyte L02 and provide evidence for the paradox effects of arsenic. Methods Human hepatocyte L02 was treated by a series of concentration of sodium arsenite or arsenic trioxide,respectively. Cytotoxicity were tested by MTT assay and colony formation assay,cellular apoptosis and cell cycle were detected by flow cytometry,chromosomal breakage were measured by micronucleus test and reactive oxygen species level and GSH contents were detected with commercial kits. Results With the increase of sodium arsenite or arsenic trioxide concentrations,cellular viability,colony formation rate and GSH contents decreased; inhibition of colony formation,cellular apoptotic rate,reactive oxygen species level and frequency of micronuclei increased,and dosed cells were both arrested in G2/ M phase of cell cycle. Conclusion Both sodium arsenite and arsenic trioxide could induce oxidative stress in human hepatocyte L02 and result in chromosomal damage,apoptosis,cell cycle arrest and cellular proliferation inhibition,suggesting that oxidative stress induction might be the common molecular mechanism of malignant transformation induced by sodium arsenite and therapeutic effectsexhibited by arsenic trioxide.
[1]BHATTACHARJEE P,BANERJEE M,GIRI A K.Role of genomic instability in arsenic-induced carcinogenicity:a review[J].Environ Int,2013,53:29-40.
[2]HUGHES M F,BECK B D,CHEN Y,et al.Arsenic exposure and toxicology:a historical perspective[J].Toxicol Sci,2011,132(2):305-332.
[3]SHEN Z X,CHEN G Q,NI J H,et al.Use of arsenic trioxide(As2O3)in the treatment of acute promyelocytic leukemia(APL):Ⅱ.Clinical efficacy and pharmacokinetics in relapsed patients[J].Blood,1997,89(9):3354-3360.
[4]WANG Z Y,CHEN Z.Acute promyelocytic leukemia:from highly fatal to highly curable[J].Blood,2008,111(5):2505-2515.
[5]屈凤莲,郝学志,秦叔逵,等.亚砷酸注射液治疗原发性肝癌的Ⅱ期多中心临床研究[J].中华肿瘤杂志,2011,33(9):697-701.
[6]MURGO A J.Clinical trials of arsenic trioxide in hematologic and slid tumors:overview of the national cancer institute cooperative research and development studies[J].Oncologist,2001,6(S2):22-28.
[7]BODE A M,DONG Z G.The paradox of arsenic:molecular mechanisms of cell transformation and chemotherapeutic effects[J].Cri Rev Oncol Hematol,2002,42(1):5-24.
[8]IVANOV V N,HEI T K.Induction of apoptotic death and retardation of neuronal differentiation of human neural stem cells by sodium arsenite treatment[J].Exper Cell Res,2013,319(6):875-887.
[9]WANG H H,XI S H,XU Y Y,et al.Sodium arsenite induces cyclooxygenase-2 expression in human uroepithelial cells through MAPK pathway activation and reactive oxygen species induction[J].Toxicol in vitro,2013,27(3):1043-1048.
[10]HELD L A,RIZZIERI D,LONG G D,et al.A phase I study of arsenic trioxide(trisenox),ascorbic acid,and bortezomib(velcade)combination therapy in patients with relapsed/refractory multiple myeloma[J].Cancer Invest,2013,31(3):172-176.
[11]CHEN L,HAN F T,QU H,et al.Combination therapy with 5-amino-4-imidazolecarboxamide riboside and arsenic trioxide in acute myeloid leukemia cells involving AMPK/TSC2/mTOR pathway[J].Die Pharmazie,2013,68(2):117-123.
[12]WANG Y,XU Y Y,WANG H H,et al.Arsenic induces mitochondria-dependent apoptosis by reactive oxygen species generation rather than glutathione depletion in Chang human hepatocytes[J].Arch Toxicol,2009,83(10):899-908.
[13]XU Y Y,WANG H H,WANG Y,et al.Effects of folate on arsenic toxicity in Chang human hepatocytes:Involvement of folate antioxidant properties[J].Toxicol Lett,2010,195(1):44-50.
[14]ALARIFI S,ALI D,ALKAHTANI S,et al.Arsenic trioxide-mediated oxidative stress and genotoxicity in human hepatocellular carcinoma cells[J].Onco Therapy,2013,6:75-84.
[15]CHIU H W,CHEN Y A,HO S Y,et al.Arsenic trioxide enhances the radiation sensitivity of androgen-dependent and-independent human prostate cancer cells[J].PLOS ONE,2012,7(2):e31579.
[16]邓志华,蔡洪培,李石,等.三氧化二砷对正常肝细胞及肝癌细胞株的影响[J].中华消化杂志,1999,19(4):227-229.
[17]RAY A,ROY S,AGARWAL S,et al.As2O3toxicity in rat hepatocytes:manifestation of caspasemediated aoptosis[J].Toxicol Indust Health,2008,24:643-653.
[18]KIM H G,KIM D J,LI S Q,et al.Polycomb(PcG)proteins,BMI1 and SUZ12,regulate arsenicinduced cell transformation[J].J Biol Chem,2012,287(38):31920-31928.
[19]STUECKLE T A,LU Y J,DAVIS M E,et al.Chronic occupational exposure to arsenic induces carcinogenic gene signaling networks and neoplastic transformation in human lung epithelial cells[J].Toxicol Appl Pharmacol,2012,261(2):204-216.
[20]BOLT H M.Current developments in toxicological research in arsenic[J].Exp Clin Sci Int online J Adv Sci,2013,12:64-74.
[21]FRUEHAUF J P,MEYSKENS F L J.Reactive oxygen species:a breath of life or death[J].Clin Cancer Res,2007,13(3):789-794.
基本信息:
DOI:10.19813/j.cnki.weishengyanjiu.2014.02.007
中图分类号:R96
引用信息:
[1]胡亚男,赵巍,陈承志,等.亚砷酸钠和三氧化二砷对人正常肝细胞增殖与凋亡效应的影响[J].卫生研究,2014,43(02):203-209.DOI:10.19813/j.cnki.weishengyanjiu.2014.02.007.
基金信息:
国家自然科学基金(No.81172632)
2014-03-30
2014-03-30