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Phage-based molecular directed evolution yields multiple tandem human IgA affibodies with intramolecular binding avidity

机译:基于噬菌体的分子定向进化产生具有分子内结合亲和力的多个串联的人IgA亲和力

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摘要

Affibodies are a group of affinity proteins that are based on a 58-amino-acid residue protein domain derived from one of the IgG-binding domains of staphylococcal protein A. A single human IgA affibody with high IgA affinity has been generated by directed evolution. It remains interesting whether tandem IgA affibody proteins could increase binding capacity. Here, we report the generation of multiple tandem IgA affibodies by directed evolution using a combinatorial phage library displaying the IgA affibody A1 and/or A2 linked with three random amino acids. These affibodies exhibited markedly increased IgA binding capacity, as shown by enzyme linked immunosorbent assay, immunoblotting and surface plasmon resonance assays. We further showed that these tandem IgA affibodies displayed preferential binding to intact IgA molecules compared to individual IgA chain, suggesting intramolecular binding avidity. Our data demonstrates that artificial multiple tandem human IgA affibodies with relevant biological binding avidity were successfully yielded by phage-based molecular evolution. These results have broad implications for the design and development of binding proteins that target important biological molecules
机译:亲和体是一组亲和蛋白,其基于衍生自葡萄球菌蛋白A的一个IgG结合域的58个氨基酸残基蛋白域。通过定向进化已产生具有高IgA亲和力的单个人IgA亲和体。串联IgA亲和体蛋白是否可以增加结合能力仍然令人感兴趣。在这里,我们报告通过使用组合噬菌体库的定向进化,产生多个串联的IgA亲和体,该噬菌体库显示了与三个随机氨基酸连接的IgA亲和体A1和/或A2。这些亲和力表现出明显增加的IgA结合能力,如酶联免疫吸附测定,免疫印迹和表面等离振子共振测定所示。我们进一步显示,与单个IgA链相比,这些串联IgA亲和力显示与完整IgA分子的优先结合,表明分子内结合亲和力。我们的数据表明,基于噬菌体的分子进化成功地产生了具有相关生物结合亲和力的人工多重串联人IgA亲和力。这些结果对靶向重要生物分子的结合蛋白的设计和开发具有广泛的意义。

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