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Inhibition of Duck Hepatitis B Virus Infection by a Myristoylated Pre-S Peptide of the Large Viral Surface Protein

机译:大病毒表面蛋白的肉豆蔻酰化的Pre-S肽抑制鸭乙型肝炎病毒感染。

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摘要

We have used the duck hepatitis B virus (DHBV) model to study the interference with infection by a myristoylated peptide representing an N-terminal pre-S subdomain of the large viral envelope protein. Although lacking the essential part of the carboxypeptidase D (formerly called gp180) receptor binding site, the peptide binds hepatocytes and subsequently blocks DHBV infection. Since its activity requires an amino acid sequence involved in host discrimination between DHBV and the related heron HBV (T. Ishikawa and D. Ganem, Proc. Natl. Acad. Sci. USA 92:6259-6263, 1995), we suggest that it is related to the postulated host-discriminating cofactor of infection.
机译:我们已经使用鸭乙型肝炎病毒(DHBV)模型研究了代表大病毒被膜蛋白N端pre-S亚域的肉豆蔻酰化肽对感染的干扰。尽管缺少羧肽酶D(以前称为gp180)受体结合位点的必需部分,但该肽结合肝细胞并随后阻断DHBV感染。由于其活性需要涉及DHBV与相关鹭HBV之间宿主区分的氨基酸序列(T. Ishikawa和D. Ganem,美国国家科学院院刊92:6259-6263,1995),因此我们建议与假定的宿主区分感染因子有关。

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