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Anti-HBs after hepatitis B immunization with plasma-derived andrecombinant DNA-derived vaccines: binding to mutant HBsAg

机译:用血浆和重组DNA疫苗接种乙型肝炎疫苗后的抗HBs:与突变型HBsAg结合

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摘要

The G145R mutant of the small S-protein is a major escape mutant of hepatitis B virus observed in natural infection, after immunization and HBIG therapy. In a previous study we found that plasma-derived and recombinant DNA-derived vaccine HBsAg reacted differently with monoclonal antibodies sensitive for the G145R change. In the present study we investigated the binding of polyclonal anti-HBs obtained after immunization with plasma vaccine and recombinant DNA vaccine to synthetic peptides (adw(2), adr) and rHBsAg (HepG2) (ayw(3); wild type and a 145R mutant). Anti-HBs binding to synthetic peptids (25-mere, 7aa overlap) from the "a"-loop was significantly reduced by the G145R substitution and by changing the amino acid sequence from adw(2) into adr. With mutant G145R rHBsAg the inhibitory activity of vaccine anti-HBs was decreased compared to rHBsAg wild type. In general only minor differences were observed between plasma vaccine and recombinant DNA vaccine related antibody responses. However, the individual heterogeneity in epitope specific reactivity with its possible consequences for protection (against escape mutants) is not reflected in an anti-HBs titer by standard anti-HBs assays. The presented differentiation in anti-HBs response after immunization may deliver new tools for evaluation of future vaccines.
机译:免疫和HBIG治疗后,在自然感染中观察到的小S蛋白的G145R突变体是乙型肝炎病毒的主要逃逸突变体。在先前的研究中,我们发现血浆衍生和重组DNA衍生的疫苗HBsAg与对G145R变化敏感的单克隆抗体反应不同。在本研究中,我们研究了血浆疫苗和重组DNA疫苗免疫后获得的多克隆抗HBs与合成肽(adw(2),adr)和rHBsAg(HepG2)(ayw(3);野生型和145R突变体)。通过G145R取代和将adw(2)的氨基酸序列更改为adr,可大大降低抗HBs与“ a”环合成肽(25-mere,7aa重叠)的结合。与野生型rHBsAg相比,突变G145R rHBsAg疫苗的抗HBs抑制活性降低。通常,在血浆疫苗和重组DNA疫苗相关的抗体反应之间仅观察到很小的差异。但是,通过标准的抗HBs检测不能在抗HBs效价中反映出表位特异性反应的个体异质性及其可能的保护后果(针对逃避突变体)。免疫后抗HBs反应的差异可能为评估未来疫苗提供了新工具。

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