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Lock-and-key motif as a concept for designing affinity adsorbents for protein purification

机译:锁匙主题作为设计用于蛋白质纯化的亲和吸附剂的概念

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The lock-and-key (LAK) motif, a common structural moiety found in subunit interfaces of glutathione S-transferases (GSTs), plays an important role in biomolecular recognition and quaternary structure integrity. Inspection of the key structural features of the LAK motif prompted the de novo design and combinatorial synthesis of a 13-membered solid-phase ligand library, employing as a lead ligand the Phe-Trz-X structure, mimicking the LAK motif. 1,3,5-Triazine (Trz) was used as the scaffold for assembly, substituted with different LAK-mimetic amino acids. De novo ligand design was effected using bioinformatics and molecular modeling and based on mimicking the interactions of the LAK motif. The library of affinity adsorbents was assessed for binding corn and human serum proteomes and purified proteins of different structure and ligand binding specificity. The results showed remarkable differences in the binding specificity of LAK-mimetic adsorbents for a wide range of proteins, as a consequence of minor changes in ligand structure. One LAK-mimetic adsorbent was integrated in a single-step purification protocol for human monoclonal anti-human immunodeficiency virus 2F5 antibody (mAb 2F5) from spiked corn extract, affording high recovery and purity. The results demonstrate that the principle of natural recognition found in the lock-and-key motif, in combination with de novo combinatorial design, may lead to synthetic affinity ligands, useful in downstream processing and proteomic research. (c) 2006 Elsevier B.V. All rights reserved.
机译:锁匙(LAK)主题是在谷胱甘肽S-转移酶(GST)的亚基界面中发现的常见结构部分,在生物分子识别和四级结构完整性中起着重要作用。对LAK基序关键结构特征的检查促进了从头设计和13元固相配体库的合成合成,采用了Phe-Trz-X结构作为主要配体,模仿了LAK基序。 1,3,5-三嗪(Trz)用作组装支架,被不同的LAK模拟氨基酸取代。从头配体设计是通过使用生物信息学和分子建模并基于模拟LAK基序的相互作用来实现的。评估了亲和吸附剂库中玉米和人血清蛋白质组以及不同结构和配体结合特异性的纯化蛋白的结合。结果表明,由于配体结构的微小变化,LAK模拟吸附剂对多种蛋白质的结合特异性差异显着。一种LAK模拟吸附剂已集成在一步纯化方案中,用于从加标的玉米提取物中提取人单克隆抗人免疫缺陷病毒2F5抗体(mAb 2F5),具有很高的回收率和纯度。结果表明,在锁键式主题中发现的自然识别原理与从头组合设计相结合,可能会导致合成亲和配体,可用于下游加工和蛋白质组学研究。 (c)2006 Elsevier B.V.保留所有权利。

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