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首页> 外文期刊>ACS Chemical Biology >Phage Selection of Chemically Stabilized alpha-Helical Peptide Ligands
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Phage Selection of Chemically Stabilized alpha-Helical Peptide Ligands

机译:化学稳定的α-螺旋肽配体的噬菌体选择

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摘要

Short alpha-helical peptides stabilized by linkages between constituent amino acids offer an attractive format for ligand development. In recent years, a range of excellent ligands based on stabilized alpha-helices were generated by rational design using alpha-helical peptides of natural proteins as templates. Herein, we developed a method to engineer chemically stabilized alpha-helical ligands in a combinatorial fashion. In brief, peptides containing cysteines in position i and i + 4 are genetically encoded by phage display, the cysteines are modified with chemical bridges to impose alpha-helical conformations, and binders are isolated by affinity selection. We applied the strategy to affinity mature an alpha-helical peptide binding beta-catenin. We succeeded in developing ligands with K-d's as low as 5.2 nM, having >200-fold improved affinity. The strategy is generally applicable for affinity maturation of any alpha-helical peptide. Compared to hydrocarbon stapled peptides, the herein evolved thioether-bridged peptide ligands can be synthesized more easily, unnatural amino acids are required and the cyclization reaction is more efficient and yields no stereoisomers. A further advantage of the thioether-bridged peptide ligands is that they can be expressed recombinantly as fusion proteins.
机译:通过组成氨基酸之间的连接稳定的短α-螺旋肽为配体的发展提供了一种有吸引力的形式。近年来,通过使用天然蛋白的α-螺旋肽作为模板的合理设计,产生了一系列基于稳定的α-螺旋的优秀配体。在这里,我们开发了一种以组合方式工程化化学稳定的α-螺旋配体的方法。简而言之,通过噬菌体展示遗传编码在位置i和i + 4处含有半胱氨酸的肽,用化学桥修饰半胱氨酸以施加α-螺旋构象,并通过亲和力选择分离结合物。我们将该策略应用于亲和力成熟的α-螺旋肽结合β-连环蛋白。我们成功地开发出K-d低至5.2 nM的配体,其亲和力提高了200倍以上。该策略通常适用于任何α-螺旋肽的亲和力成熟。与烃钉合肽相比,本文进化的硫醚桥连肽配体可以更容易地合成,需要非天然氨基酸并且环化反应更有效并且不产生立体异构体。硫醚桥连的肽配体的另一个优点是它们可以作为融合蛋白重组表达。

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