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首页> 外文期刊>Protein engineering design & selection: PEDS >Modular protein switches derived from antibody mimetic proteins
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Modular protein switches derived from antibody mimetic proteins

机译:源自抗体模拟蛋白的模块化蛋白开关

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Protein switches have potential applications as biosensors and selective protein therapeutics. Protein switches built by fusion of proteins with the prerequisite input and output functions are currently developed using an ad hoc process. A modular switch platform in which existing switches could be readily adapted to respond to any ligand would be advantageous. We investigated the feasibility of a modular protein switch platform based on fusions of the enzyme TEM-1 beta-lactamase (BLA) with two different antibody mimetic proteins: designed ankyrin repeat proteins (DARPins) and monobodies. We created libraries of random insertions of the gene encoding BLA into genes encoding a DARPin or a monobody designed to bind maltose-binding protein (MBP). From these libraries, we used a genetic selection system for beta-lactamase activity to identify genes that conferred MBP-dependent ampicillin resistance to Escherichia coli. Some of these selected genes encoded switch proteins whose enzymatic activity increased up to 14-fold in the presence of MBP. We next introduced mutations into the antibody mimetic domain of these switches that were known to cause binding to different ligands. To different degrees, introduction of the mutations resulted in switches with the desired specificity, illustrating the potential modularity of these platforms.
机译:蛋白质开关作为生物传感器和选择性蛋白质治疗剂具有潜在的应用。当前,使用特设方法开发了通过融合具有必要的输入和输出功能的蛋白质而构建的蛋白质开关。在其中可以容易地使现有开关适应任何配体响应的模块化开关平台将是有利的。我们研究了基于酶TEM-1β-内酰胺酶(BLA)与两种不同的抗体模拟蛋白(设计的锚蛋白重复蛋白(DARPins)和单克隆抗体)融合的模块化蛋白转换平台的可行性。我们创建了将BLA编码基因随机插入到DARPin编码基因或设计为结合麦芽糖结合蛋白(MBP)的单体的基因库。从这些库中,我们使用了一种针对β-内酰胺酶活性的基因选择系统来鉴定赋予MBP依赖性氨苄青霉素对大肠杆菌耐药性的基因。这些选择的基因中的一些编码开关蛋白,在MBP存在下其酶促活性增加至14倍。接下来,我们将突变引入这些开关的抗体模拟域中,这些突变已知会导致与不同配体的结合。在不同程度上,引入突变导致开关具有所需的特异性,说明了这些平台的潜在模块性。

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