首页> 外文期刊>Journal of Biochemistry >Ig L-chain Shuffling for Affinity Maturation of Phage Library-derived Human Anti-human MCP-1 Antibody Blocking its Chemotactic Activity
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Ig L-chain Shuffling for Affinity Maturation of Phage Library-derived Human Anti-human MCP-1 Antibody Blocking its Chemotactic Activity

机译:Ig L链改组的噬菌体库派生的人类抗人类MCP-1抗体亲和力成熟阻碍其趋化活性。

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摘要

Monocyte chemotactic protein-1 (MCP-1, CC-chemokine ligand 2; CCL2) is involved in the development of various forms of chronic inflammations. Employing the naive human single-chain Fv displaying phage library, we established seven MCP-1-specific scFvs. The MC8 and MC32 clones exhibited blocking activity for the MCP-1-induced chemotaxis of THP-1 cells, in spite of their monovalency. The analysis of V gene usage showed that all clones bore the identical Vh1 gene, IGHV1-24*01, with variable DJ joining sequences, while their Vl usage was relatively varied, suggesting the preferential contribution of the Vh gene. Based on these findings, to minimize the deteriorative influences on the MCP-1 specificity of MC32, we aimed to achieve the affinity maturation of MC32 using MC32 L-chain shuffling library and select MC32 variants. Most MC32 variants increased their affinity by reducing the koff value with no influence of the antigen specificity. MC32 variants #22 or #56 showed ∼15-fold higher affinity than MC32, indicating that the L-chain shuffling library is useful if the Vh is dominantly involved in the determination of the antigen specificity.
机译:单核细胞趋化蛋白-1(MCP-1,CC趋化因子配体2; CCL2)参与各种形式的慢性炎症的发展。利用天真的人类单链Fv展示噬菌体库,我们建立了七个MCP-1特异性scFv。尽管MC8和MC32单价存在,但它们仍对MCP-1诱导的THP-1细胞趋化性具有阻断活性。对V基因使用情况的分析表明,所有克隆都具有相同的Vh1基因IGHV1-24 * 01,具有可变的DJ连接序列,而它们的V1使用情况则相对不同,表明Vh基因具有优先作用。基于这些发现,为了最小化对MC32的MCP-1特异性的不利影响,我们旨在使用MC32 L链改组文库并选择MC32变体来实现MC32的亲和力成熟。大多数MC32变体通过降低k off 值来增加其亲和力,而不会影响抗原特异性。 MC32变体#22或#56的亲和力比MC32高约15倍,这表明如果Vh主要参与抗原特异性的确定,则L链改组文库很有用。

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