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重组8型腺相关病毒介导HBV急性感染树鼩模型建立
引用本文:曾扬,吴小红,胡靓雅,刘晨风,于虹,郭彦,周勇,孙世惠,周育森. 重组8型腺相关病毒介导HBV急性感染树鼩模型建立[J]. 中国实验动物学报, 2013, 0(3): 36-41,F0002
作者姓名:曾扬  吴小红  胡靓雅  刘晨风  于虹  郭彦  周勇  孙世惠  周育森
作者单位:[1]军事医学科学院微生物流行病研究所,北京100071 [2]军事医学科学院野战输血研究所,北京100850
基金项目:十二五国家科技重大专项[2012ZX10004502].
摘    要:目的利用重组8型腺相关病毒介导1.3拷贝HBV基因组(1.3HBV,ayw亚型)在树鼩肝脏表达,建立HBV急性感染树鼩模型。方法通过大腿内侧静脉注射将携带有1.3 HBV的重组8型腺相关病毒(recombi-nant adeno-associated virus 8,rAAV8-1.3HBV)导入树鼩肝脏,通过ELISA检测树鼩血清中HBsAg、HBeAg、HBsAb、HBeAb、HBcAb,荧光定量PCR检测树鼩肝脏和血清中HBV DNA,全自动生化分析仪检测血清中ALT水平,并观察感染后肝脏的病变情况。结果 HBV感染主要血清标志物1~2周内均检测阳性;30 d后肝组织仍可检测到病毒抗原阳性细胞;55 d时肝组织HBV DNA拷贝数仍可达到104~105;树鼩血清中HBV DNA拷贝数持续一个月高于正常组;肝组织炎细胞略增多,血清ALT水平持续升高。结论 rAAV8所携带的HBV基因组高效专一导入树鼩肝细胞并复制表达,成功建立HBV急性感染树鼩模型,为进一步探索rAAV8树鼩慢性感染模型打下一定的基础。

关 键 词:树鼩  乙型肝炎病毒  重组8型腺相关病毒  HBV急性感染模型

Establishment of a tree shrew infection by transduction with virus 8 carrying 1.3 model of acute hepatitis B virus a recombinant adeno-associated copies of HBV genome
ZENG Yang,WU Xiao-hong,HU Jing-ya,LIU Chen-feng,YU Hong,GUO Yan,ZHOU Yong,SUN Shi-hui,ZHOU Yu-sen. Establishment of a tree shrew infection by transduction with virus 8 carrying 1.3 model of acute hepatitis B virus a recombinant adeno-associated copies of HBV genome[J]. Acta Laboratorium Animalis Scientia Sinica, 2013, 0(3): 36-41,F0002
Authors:ZENG Yang  WU Xiao-hong  HU Jing-ya  LIU Chen-feng  YU Hong  GUO Yan  ZHOU Yong  SUN Shi-hui  ZHOU Yu-sen
Affiliation:1. Institute of Microbiology and Epidemiology, Academy of Military Medical Sciences, Beijing 100071, China; 2. Institute of Transfusion Medicine, Academy of Military Medical Sciences, Beijing 100850)
Abstract:Objective To establish a tree shrew model of acute hepatitis B virus infection by injection of a recombinant adeno-assoeiated virus 8 vector carrying 1.3 copies of HBV genome (ayw subtype) (rAAV8-1.3 HBV)into the liver of tree shrews. Methods Serum and liver tissues were collected at indicated times after i. v. injection of rAAV8-1.3 HBV into the tree shrews. The HBsAg, BeAg, HBsAb, HBeAb, HBcAb, ALT and HBV virus load were examined by ELISA and real-time PCR, respectively. The expression of HBcAg and pathological changes in the liver were also observed after the rAAV8-1.3 HBV infection. Results Markers of serum HBV were all positive 2 weeks after and HBcAg-positive hepatocytes were even detected in the liver 55 days after rAAV8-1.3 HBV injection. The copies of HBV DNA in liver reached 104 - 105 at 55 days after rAAVS-1.3HBV injection. Serum HBV DNA could be detected for over one month. Mild pathological changes with elevated ALT were observed after rAAV8-1.3 HBV injection. Conclusions A tree shrew model of acute HBV infection has been successfully established with the recombinant adeno-assoeiated virus 8 carrying 1.3 copies of HBV genome (rAAV8-1.3 HBV). Our study provides a novel and useful small animal model for the research of immuno- pathologic mechanism as well as the evaluation of vaccine and anti-HBV agents.
Keywords:Tree shrew  Hepatitis B virus (HBV)  Recombinant adeno-associated virus 8 (rAAV8)  Acute hepatitis B virus Infection, Animal model
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