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Hepatitis B virus-neutralizing anti-pre-S1 human antibody fragments from large naive antibody phage library.

机译:来自大型天真抗体噬菌体库的中和乙肝病毒的抗S1前人类抗体片段。

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We report the construction of a large nonimmunized human phage antibody library in single-chain variable region fragment (scFv) format, which allowed the selection of antibodies that neutralize hepatitis B virus (HBV) in vitro. We generated 1.1 x 10(10) independent scFv clones using the cDNA of functional variable (V) gene segments of heavy and light chains purified from the peripheral blood mononuclear cells of 50 nonimmunized human donors. Using BIAcore, we selected two clones that recognized pre-S1 and neutralized pre-S1 and HBV binding to Chang liver cells. Clone G10 had the highest affinity (K(D)=1.69 x 10(-7)M), which was higher than that of clone 1E4 that was generated previously from a heavy chain-shuffled immune library. The off-rates of clones were within 10(-3)s(-1) as determined by BIAcore and were comparable to those of antibodies derived from a normal secondary immune response. In the inhibition assays of pre-S1 and virus binding to Chang liver cells using flow cytometry and the polymerase chain reaction, G10 had better neutralizing activity than 1E4. The new phage library may be a valuable source of antibodies with reasonable affinities to different targets, and the anti-pre-S1 G10 may be a good candidate for immunoprophylaxis against HBV infection.
机译:我们报告了单链可变区片段(scFv)格式的大型非免疫人类噬菌体抗体库的构建,该库允许选择在体外中和乙型肝炎病毒(HBV)的抗体。我们使用从50个未免疫人类供体的外周血单核细胞中纯化的重链和轻链功能可变(V)基因区段的cDNA生成了1.1 x 10(10)个独立的scFv克隆。使用BIAcore,我们选择了两个克隆,它们识别pre-S1并中和pre-S1和HBV与Chang肝细胞的结合。克隆G10具有最高的亲和力(K(D)= 1.69 x 10(-7)M),高于先前从重链改组的免疫文库中生成的克隆1E4的亲和力。由BIAcore确定,克隆的解离速率在10(-3)s(-1)范围内,可与源自正常次级免疫反应的抗体相当。在使用流式细胞仪和聚合酶链反应进行的前S1抑制和病毒与Chang肝细胞结合的抑制分析中,G10具有比1E4更好的中和活性。新的噬菌体文库可能是对不同靶标具有合理亲和力的抗体的重要来源,而抗S1前G10抗体可能是预防HBV感染的好方法。

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