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Human recombinant antibodies specific for hepatitis C virus core and envelope E2 peptides from an immune phage display library

被引:25
作者
Chan, SW
Bye, JM
Jackson, P
Allain, JP
机构
[1] MRC,MOL IMMUNOPATHOL UNIT,MRC CTR,CAMBRIDGE CB2 2QH,ENGLAND
[2] UNIV CAMBRIDGE,CTR MRC,DIV TRANSFUS MED,DEPT HAEMATOL,CAMBRIDGE CB2 2QH,ENGLAND
[3] E ANGLIAN BLOOD TRANSFUS CTR,CAMBRIDGE CB2 2PT,ENGLAND
来源
JOURNAL OF GENERAL VIROLOGY | 1996年 / 77卷
关键词
D O I
10.1099/0022-1317-77-10-2531
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
Hepatitis C virus (HCV) is the aetiological agent responsible for most cases of non-A non-B hepatitis. Hepatitis C is a disease of clinical importance because of its high infection rate in blood donors and its persistence as chronic infections which may lead to cirrhosis and hepatocellular carcinoma in the long term. The variability of the HCV genome has posed difficulties in serological detection and vaccine design. The recent advance in phage technology offers a means of cloning human anti-HCV antibodies of a defined specificity that may have potential therapeutic use. We now report the generation of a phage display library using the V-H genes of a HCV-infected patient and the V-L genes of two non-immune individuals. From this library we were able to obtain specific IgG single-chain Fvs (scFvs) that recognize viral core and envelope proteins by selection on synthetic peptides derived from the core sequence PKARRPEGRTWAQPG and the envelope E2 sequence RPIDDFDQGWGPITY. The specificity of the scFvs was demonstrated by their specific reactions with homologous peptides in ELISA and the specific blocking of scFv binding by homologous peptides, in a dose-dependent manner, in inhibition ELISA. The binding of the anti-core 4c2 to homologous peptide was blocked by HCV-positive human sera in an antibody-concentration-dependent manner, suggesting that the scFv recognizes a similar if not identical epitope to those of one or more of the polyclonal antibodies present in the sera.
引用
收藏
页码:2531 / 2539
页数:9
相关论文
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