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乙型肝炎转基因小鼠品系C57-TgN(HBV adr2.0)SMMU的生物学特征
引用本文:訾晓渊,姚玉成,熊俊,金艳花,叶煦亭,李建秀,刘红,朱海英,王新民,倪文君,余宏宇,丛文铭,胡以平. 乙型肝炎转基因小鼠品系C57-TgN(HBV adr2.0)SMMU的生物学特征[J]. 第二军医大学学报, 2002, 23(11): 1179-1183
作者姓名:訾晓渊  姚玉成  熊俊  金艳花  叶煦亭  李建秀  刘红  朱海英  王新民  倪文君  余宏宇  丛文铭  胡以平
作者单位:1. 第二军医大学基础医学部细胞生物学教研室,上海,200433
2. 长征医院病理科
3. 东方肝胆外科医院病理科
基金项目:国家“九五”攻关项目(TJ99-LA01),国家自然科学 基金资助项目(39670811),上海市科学技术发展基金项目 (994919033).
摘    要:目的:评价乙肝转基因小鼠品系C57-TgN(HBV adr2.0)SMMU生物学特征的稳定性。方法:以F6代乙肝转基因小鼠C57-TgN(HBV adr2.0)SMMU为研究对象,采用基因组DNA PCR,血清ELISA检测,Western印迹分析,免疫组织化学,血清DNA PCR,透射电镜和H-E染色的方法分析HBV基因在转基因小鼠中的整合,表达,复制和组织这变化。结果:F6代乙肝转基因小鼠基因组中稳定整合有HBV基因,肝组织中可检测用HBsAg,HBcAg和X蛋白3种病毒蛋白,血清中HBsAg和HBeAg的表达率分别为19.54%和3.39%,且在血清和肝组织中存在病毒NA和病毒样颗粒;长期的病毒DNA整合,表达和复制可以引起转基因小鼠肝,肺等组织的病理性损伤。结论:乙肝转基因小鼠品系C57-TgN(HBV adr2.0)SMMU具有基因组中稳定整合病毒DNA,血清和肝组织中有病毒蛋白表达和病毒复制的特征,并具有一定的组织这变化,作为生物医药研究的实验动物模型具有推广应用价值。
关 键 词:乙型肝炎病毒 转基因小鼠 免疫组织化学 病理学
文章编号:0258-879X(2002)11-1179-05
修稿时间:2002-09-30

Biological characters of hepatitis B virus transgenic mice strain C57-TgN(HBV adr2.0)SMMU
ZI Xiao-Yuan,YAO Yu-Cheng,XIONG Jun,JIN Yan-Hua,YE Xu-Ting,LI Jian-Xiu,LIU Hong,ZHU Hai-Ying,WANG Xin-Min,NI Wen-Jun,YU Hong-Yu,CONG Wen-Ming,HU Yi-Ping. Biological characters of hepatitis B virus transgenic mice strain C57-TgN(HBV adr2.0)SMMU[J]. Former Academic Journal of Second Military Medical University, 2002, 23(11): 1179-1183
Authors:ZI Xiao-Yuan  YAO Yu-Cheng  XIONG Jun  JIN Yan-Hua  YE Xu-Ting  LI Jian-Xiu  LIU Hong  ZHU Hai-Ying  WANG Xin-Min  NI Wen-Jun  YU Hong-Yu  CONG Wen-Ming  HU Yi-Ping
Abstract:Objective:To evaluate the biological characters of C57-TgN(HBV adr2.0)SMMU transgenic mice. Methods: Integration,expression,replication and histology change of hepatitis B virus gene in F6 transgenic mice were estimated by ge-nomic DNA PCR,Western blotting,ELISA,immunohistochemistry,serum DNA PCR,transmission electron microscopy and H-E staining. Results: Hepatitis B virus gene was integrated into F6 C57-TgN(HBV adr2. 0)SMMU transgenic mice and expressed HBsAg,HBcAg and X protein in liver tissue. HBsAg and HBeAg were expressed in serum of 19. 54% and 3. 39% F6 transgenic mice. Hepatitis B virus were replicated in serum and liver tissue of transgenic mice. Long-term integration,expression and replication of hepatitis B virus gene induced pathological lesion of transgenic mice liver and lung. Conclusion: C57-TgNCHBV adr2. 0)SMMU transgenic mice line has the biological characters including integration of hepatitis B virus gene into genomic DNA,expression and replication of hepatitis B virus gene in serum and liver, and histological change in liver and lung. It is a valuable animal system to study pathogenesis, treatment and prevention of hepatitis B virus.
Keywords:hepatitis B virus  transgenic mouse  immunohistochemistry  pathology
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