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首页> 外文期刊>Electrophoresis: The Official Journal of the International Electrophoresis Society >Application of plug-plug technique to ACE experiments for discovery of peptides binding to a larger target protein: A model study of calmodulin-binding fragments selected from a digested mixture of reduced BSA
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Application of plug-plug technique to ACE experiments for discovery of peptides binding to a larger target protein: A model study of calmodulin-binding fragments selected from a digested mixture of reduced BSA

机译:随插即用技术在ACE实验中发现与较大目标蛋白结合的肽的应用:钙调蛋白结合片段的模型研究,该片段选自还原的BSA的消化混合物

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摘要

To discover peptide ligands that bind to a target protein with a higher molecular mass, a concise screening methodology has been established, by applying a "plug-plug" technique to ACE experiments. Exploratory experiments using three mixed peptides, mastoparan-X, β-endorphin, and oxytocin, as candidates for calmodulin-binding ligands, revealed that the technique not only reduces the consumption of the protein sample, but also increases the flexibility of the experimental conditions, by allowing the use of MS detection in the ACE experiments. With the plug-plug technique, the ACE-MS screening methodology successfully selected calmodulin-binding peptides from a random library with diverse constituents, such as protease digests of BSA. Three peptides with Kd values between 8-147 μM for calmodulin were obtained from a Glu-C endoprotease digest of reduced BSA, although the digest showed more than 70 peaks in its ACE-MS electropherogram. The method established here will be quite useful for the screening of peptide ligands, which have only low affinities due to their flexible chain structures but could potentially provide primary information for designing inhibitors against the target protein.
机译:为了发现与更高分子量的目标蛋白结合的肽配体,通过将“即插即用”技术应用于ACE实验,建立了简洁的筛选方法。使用Masoparan-X,β-内啡肽和催产素这三种混合肽作为钙调蛋白结合配体的候选者的探索性实验表明,该技术不仅减少了蛋白质样品的消耗,还增加了实验条件的灵活性,通过允许在ACE实验中使用MS检测。通过即插即用技术,ACE-MS筛选方法成功地从具有各种成分(例如BSA蛋白酶消化物)的随机文库中选择了钙调蛋白结合肽。从还原的BSA的Glu-C内切蛋白酶消化物中获得了钙调蛋白Kd值在8-147μM之间的三种肽,尽管该消化物在其ACE-MS电泳图中显示了70多个峰。此处建立的方法对于筛选肽配体将非常有用,肽配体由于其柔性链结构而仅具有低亲和力,但可能为设计针对靶蛋白的抑制剂提供主要信息。

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