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本帖最后由 风雨不动 于 2012-4-14 14:47 编辑
J Virol. 2012 Feb 1. [Epub ahead of print]
Amino acid substitutions at the positions 122 and 145 of hepatitis B surface antigen (HBsAg) determine the antigenicity and immunogenicity of HBsAg and influence in vivo HBsAg clearance.Wu C, Deng W, Deng L, Cao L, Qin B, Li S, Wang Y, Pei R, Yang D, Lu M, Chen X.
SourceWuhan Institute of Virology, Chinese Academy of Sciences, Wuhan, China.
AbstractA variety of amino acid (8) substitutions such as K122I and G145R have been identified around or within the "a" determinant of hepatitis B surface antigen (HBsAg), impair HBsAg secretion and antibody binding and may be responsible for immune escape in patients. In this study, we examined how different substitutions at aa positions 122 and 145 of HBsAg influence HBsAg expression, secretion, and recognition by anti-HBs antibodies. The results showed that the hydrophobicity, the presence of the phenyl group, and the charges in the side chain of the aa residues at position 145 reduced HBsAg secretion and impaired reactivity with anti-HBs antibodies. Only the substitution K122I at the position 122 affected HBsAg secretion and recognition by anti-HBs antibodies. Genetic immunization in mice demonstrated that priming of anti-HBs antibody response was strongly impaired by the substitutions K122I, G145R, and others like G145I, G145W, and G145E. Mice preimmunized with wtHBsAg or variant HBsAg (vtHBsAg) were challenged by hydrodynamic injection (HI) with a replication competent hepatitis B virus (HBV) clone. HBsAg persisted in peripheral blood for at least 3 days after HI in mice preimmunized with vtHBsAg but undetectable in mice preimmunized with wtHBsAg indicating vtHBsAg may fail to induce proper immune responses for efficient HBsAg clearance. In conclusion, the biochemical properties of aa residues at positions 122 and 145 of HBsAg have a major impact on the antigenicity and immunogenecity. In addition, the presence of proper anti-HBs antibodies is indispensable for neutralization and clearance of HBsAg during HBV infection.
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