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Design of protein conformational switches

机译:蛋白质构象开关的设计

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Protein conformational switches are ubiquitous in nature and often regulate key biological processes. To design new proteins that can switch conformation, protein designers have focused on the two key components of protein switches: the amino acid sequence must he compatible with the multiple target states and there must be a mechanism for perturbing the relative stability of these states. Proteins have been designed that can switch between folded and disordered states, between distinct folded states and between different aggregation states. A variety of trigger mechanisms have been used, including pH shifts, post-translational modification and ligand binding. Recently, computational protein design methods have been applied to switch design. These include algorithms for designing novel ligand-binding sites and simultaneously optimizing a sequence for multiple target structures.
机译:蛋白质构象开关在自然界无处不在,并经常调节关键的生物学过程。为了设计可以转换构象的新蛋白质,蛋白质设计人员将重点放在蛋白质转换的两个关键组成部分上:氨基酸序列必须与多个靶标状态兼容,并且必须存在一种机制来扰乱这些状态的相对稳定性。已经设计了可以在折叠状态和无序状态之间,不同折叠状态之间以及不同聚集状态之间切换的蛋白质。已经使用了多种触发机制,包括pH改变,翻译后修饰和配体结合。近来,计算蛋白质设计方法已经应用于开关设计。这些包括用于设计新颖的配体结合位点并同时针对多个靶结构优化序列的算法。

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