Jacinta Skelly scite author profile

The immunoprophylaxis of hepatitis B is hampered by the lack of a technique for growing hepatitis B virus (HBV) in tissue culture. Plasma from persistently infected individuals, one source of viral antigen, contains characteristic 22-nm spherical particles which share a common antigen (the hepatitis B surface antigen or HBsAg) with the outer envelope of the 42-nm double-shelled DNA virus. Highly purified inactivated 22-nm particles have been shown to be safe and to confer protective immunity against HBV in a recent large-scale clinical trial. We have already described the extraction from the particles of a complex of two proteins which are antigenic determinants of HBV--the polypeptide with molecular weight (MW) between 22,000 and 24,000 (called p23) and the glycosylated polypeptide (called gp28) with MW in the range 26,000--29,000 which is thought to be the glycosylated form of p23. We now report the preparation from this complex of water-soluble protein micelles which may be a suitable basis for a second-generation hepatitis B vaccine.

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Hepatitis B surface antigen produced by a human hepatoma cell line

Skelly

Copeland

Howard

et al. 1979

Nature

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Jacinta Skelly

Analysis of Hepatitis B Surface Antigen Components Solubilized with Triton X-100

Hepatitis B polypeptide vaccine preparation in micelle form

Hepatitis B surface antigen produced by a human hepatoma cell line

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