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The Properties of an HBV Surface Antigen Protein Carrying the Binding Site for the Receptor of Hepatocytes——Its Formation of Surface Antigen Particles and Secretion From Discrete Cell Lines 被引量:1

The Properties of an HBV Surface Antigen Protein Carrying the Binding Site for the Receptor of Hepatocytes——Its Formation of Surface Antigen Particles and Secretion From Discrete Cell Lines
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摘要 A human hepatitis B virus (HBV) gene, which encodes the major surface antigen protein(S protein) carrying the hepatocyte receptor-binding site, was constructed with site-directed mutagenesis and in vitro recombination. When expressed in monkey kidney cell line COS-M6, this gene product (S309 protein) formed surface antigen (HBsAg) particles and secreted from the cells. It was stable within the cells and in the culture medium and could be immunoprecipitated with antisera directed against plasma-derived HBsAg or synthetic preS1 polypeptide. Isopycnic CsCl gradient centrifugation showed that the density of S309 protein particles (1.25 g/ml) was slightly higher than that of S protein particles. The S309 protein was readily secretable from hepatoma cell lines, and the amount secreted was comparable to that of the S protein. By contrast, only about 10% of the S309 protein was secreted from COS-M6 cells, and its appearance in culture medium was delayed. The efficiency of the secretion of the S309 protein can be improved when it is coexpressed with the S protein. A human hepatitis B virus (HBV) gene, which encodes the major surface antigen protein(S protein) carrying the hepatocyte receptor-binding site, was constructed with site-directed mutagenesis and in vitro recombination. When expressed in monkey kidney cell line COS-M6, this gene product (S309 protein) formed surface antigen (HBsAg) particles and secreted from the cells. It was stable within the cells and in the culture medium and could be immunoprecipitated with antisera directed against plasma-derived HBsAg or synthetic preS1 polypeptide. Isopycnic CsCl gradient centrifugation showed that the density of S309 protein particles (1.25 g/ml) was slightly higher than that of S protein particles. The S309 protein was readily secretable from hepatoma cell lines, and the amount secreted was comparable to that of the S protein. By contrast, only about 10% of the S309 protein was secreted from COS-M6 cells, and its appearance in culture medium was delayed. The efficiency of the secretion of the S309 protein can
出处 《Science China Chemistry》 SCIE EI CAS 1993年第6期685-692,共8页 中国科学(化学英文版)
基金 This research was supported in part by U.S.Public Health Service Grants CA-07175 and CA-22443 from the National Institutes of Health
关键词 HEPATITIS B virus hepatoeyte RECEPTOR binding site surface ANTIGEN partiele secretability. hepatitis B virus, hepatoeyte receptor binding site, surface antigen partiele, secretability.
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  • 1Alfredo Alberti,Wolfram H. Gerlich,Klaus-Hinrich Heermann,Patrizia Pontisso.Nature and display of hepatitis B virus envelope proteins and the humoral immune response[J]. Springer Seminars in Immunopathology . 1990 (1)
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  • 4Yu,X M.The properties of an HBV surface antigen protein carrying the (preS) binding site for the receptor of hepatocytes:its coexpression with the major surface antigen protein in COSM6 cells. Acta Biochimica et Biophysica Sinica . 1992
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  • 7Alberti,A,Gerlich,WH,Heermann,KH,Pontisso,P.Nature and display of hepatitis B virus envelope proteins and the humoral immune response. Springer Semin Immunpathol . 1990
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