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二甲基苯蒽和苯并(a)芘对小鼠肝脏金属硫蛋白及氧化损伤的诱导作用
引用本文:张宝旭,阮明,邱飞婵,贾凤兰,魏雪涛,蒋建军,尚兰琴.二甲基苯蒽和苯并(a)芘对小鼠肝脏金属硫蛋白及氧化损伤的诱导作用[J].环境科学学报,2002,22(6):764-767.
作者姓名:张宝旭  阮明  邱飞婵  贾凤兰  魏雪涛  蒋建军  尚兰琴
作者单位:北京大学公共卫生学院环境医学研究所毒理学系,北京,100083
基金项目:国家自然科学基金资助课题 (No .39970 6 4 8)
摘    要:观察两种致癌性多环芳烃化合物二甲基苯蒽(DMBA)和苯并(a)芘(BaP)对小鼠肝脏脂质过氧化产物和金属硫蛋白含量的影响。选用雄性C57BL/OLA129小鼠,观察DMBA和BaP各50mg/kg一次腹腔注射染毒后24、48、72和144h后的动物肝脏重量、金属硫蛋白(MT)含量和脂质过氧化程度的变化。MT测定采用镉-血红蛋白亲和分析法;脂质过氧化指标为硫代巴比妥酸测定丙二醛法。结果表明,DMBA和BaP均能引起小鼠肝脏重量增加、MT含量增加和MDA含量增加。随着DMBA和BaP染毒后的时间延长小鼠肝脏的重量不断增加,呈现时间效应关系。小鼠肝脏MT的含量在染毒后24和48h后明显增加1倍。肝脏MDA的含量增加在染毒后24h后达到高峰。本研究观察到DMBA和Bap可以MT增加。MT的增加与MDA的增加呈现一定平行的关。提示MT诱导可能与多环芳烃化合物所致的氧化损伤有关。
关 键 词:肝脏  氧化损伤  金属硫蛋白  二甲基苯蒽  苯并(a)芘  脂质过氧化  致癌物质  环境污染物  毒性机理  多环芳烃
文章编号:0253-2468(2002)-06-0764-04
收稿时间:1/9/2002 12:00:00 AM
修稿时间:2002年1月9日

Effect of 12-dimethylbenz(a)athrancene and benzo(a)pyrene on metallothionein expression and lipid peroxidation in mouse liver
ZHANG Baoxu,RUAN Ming,QIU Feichan,JIA Fenglan,WEI Xuetao,JIANG Jianjun and SHANG Lanqin.Effect of 12-dimethylbenz(a)athrancene and benzo(a)pyrene on metallothionein expression and lipid peroxidation in mouse liver[J].Acta Scientiae Circumstantiae,2002,22(6):764-767.
Authors:ZHANG Baoxu  RUAN Ming  QIU Feichan  JIA Fenglan  WEI Xuetao  JIANG Jianjun and SHANG Lanqin
Institution:Department of Toxicology, School of Public Health, Beijing University, Beijing 100083, CHINA,Department of Toxicology, School of Public Health, Beijing University, Beijing 100083, CHINA,Department of Toxicology, School of Public Health, Beijing University, Beijing 100083, CHINA,Department of Toxicology, School of Public Health, Beijing University, Beijing 100083, CHINA,Department of Toxicology, School of Public Health, Beijing University, Beijing 100083, CHINA,Department of Toxicology, School of Public Health, Beijing University, Beijing 100083, CHINA and Department of Toxicology, School of Public Health, Beijing University, Beijing 100083, CHINA
Abstract:To study the induction of metallothionein (MT) and lipid peroxidation by two polycyclic aromatic hydrocarbons (PAHs), 7,12 dimethylbenza]athrancene (DMBA) and benzoa]pyrene (BaP) in mice liver. Male mice were treated with DMBA or BaP i.p. at the dose of 50?mg/kg body weight for 0, 24, 48, 72 and 144?h, respectively. Liver MT was measured by the cadmium/hemoglobin saturation assay. Lipid peroxidation product (malondialdehyde, MDA) was measured as thiobarbituric acid reactive substances. After DMBA or BaP treatment, mice liver weight, MT and MDA increased in amount. Liver boby weight ratio increased significantly in a time dependent manner. MT was significantly induced vs control after 24?h with PAHs treatment. Liver MDA level was elevated one fold after 24?h treatment. Liver MT has been induced by PAHs. The correlation between MT expression and MDA level suggest that MT may be related with oxidative stress caused by PAHs.
Keywords:metallothionein  7  12  dimethylbenz[a]athrancene  benzo[a]pyrene  lipid peroxidation  
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