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摘要:
Hepatitis B virus (HBV) is one of the major causes of chronic hepatitis, cirrhosis and liver cancer. In combating HBV infections, HBV diagnosis and vaccination are therefore critical. The hepatitis B virus surface antigen (HBsAg) is a key target molecule in developing vaccines and diagnostic systems. To date, although HBsAg has been expressed in bacteria, yeasts and mammalian cells, there are still limitations in the existing ones, which leave the necessity for searching new HBsAg production methods. In this study, a simple phage display-based method was developed to produce the purified full-length HBsAg molecules for further immunization studies. For this purpose, the HBsAg coding gene was cloned into a pCANTAB5E phagemid vector and expressed on the surface of M13 filamentous phages. The HBsAg-expressing phage nanosystem was then used as immunization agent in BALB/cJ mice. The ELISA results for sera obtained from mice immunized with HBsAg-displaying phage particles revealed an immune response against HBsAg. These results demonstrate the potential use of a full-length antigen to be displayed on phages as cost effective adjuvant-free immunization agents as an alternative to the highly purified and more expensive antigens conjugated with carrier molecules.
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篇名 Cost effective filamentous phage based immunization nanoparticles displaying a full-length hepatitis B virus surface antigen
来源期刊 生命科学与技术进展(英文) 学科 医学
关键词 PHAGE Display HEPATITIS B Virus Surface ANTIGEN Protein Expression PHAGE IMMUNIZATION Nano Vector System
年,卷(期) 2014,(1) 所属期刊栏目
研究方向 页码范围 46-53
页数 8页 分类号 R73
字数 语种
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研究主题发展历程
节点文献
PHAGE
Display
HEPATITIS
B
Virus
Surface
ANTIGEN
Protein
Expression
PHAGE
IMMUNIZATION
Nano
Vector
System
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研究分支
研究去脉
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相关学者/机构
期刊影响力
生命科学与技术进展(英文)
月刊
2156-8456
武汉市江夏区汤逊湖北路38号光谷总部空间
出版文献量(篇)
314
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0
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0
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