Expression and purification of single-chain anti-HBx antibody in Escherichia coli

被引:0
|
作者
G. Zhou
Kang-Da Liu
Hui-Chuan Sun
Ya-Hua Chen
Zhao-You Tang
Clause H. Schröder
机构
[1] Liver Cancer Institute,
[2] Shanghai Medical University,undefined
[3] Shanghai,undefined
[4] P.R. China,undefined
[5] Shanghai Institute of Biochemistry,undefined
[6] Academia Sinica,undefined
[7] Shanghai,undefined
[8] P.R. China,undefined
[9] German Cancer Research Center,undefined
[10] Heidelberg,undefined
[11] Germany,undefined
[12] Center Laboratory of Zhongshan Hospital,undefined
[13] Shanghai Medical University,undefined
[14] Shanghai 200032,undefined
[15] P.R. China Tel. +86 21 64041990 (2295),undefined
来源
Journal of Cancer Research and Clinical Oncology | 1997年 / 123卷
关键词
Key words Hepatocellular carcinoma (HCC); Targeting therapy; Single-chain antibody; Immobilized metal chelate affinity chromatography;
D O I
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中图分类号
学科分类号
摘要
 Monoclonal antibodies have been widely used in tumor targeting studies with promising results. However, their clinical application has been limited by heterogeneity and macro-molecular movement of murine antibody. In this study, the variable-region (heavy- and light-chain) fragments of anti-HBx monoclonal antibody were enriched by the polymerase chain reaction. The expression vector, which included a 6x histidine sequence in the 3′ terminus of the HBx single-chain antibody (sFv) was recombined with a linker sequence (KLGGGGFSGA) between the variable regions. The expression product from Escherichia coli fused with 6xHis was purified by nickel (Ni2+) nitrilotriacetate chelating resin. The results of enzyme-linked immunosorbent assay and Western blotting showed that sFv had binding affinity with HBxAg, suggesting that it could become a novel targeting carrier in clinical trials.
引用
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页码:609 / 613
页数:4
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