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首页> 外文期刊>The Journal of Chemical Physics >Structural flexibility of intrinsically disordered proteins induces stepwise target recognition
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Structural flexibility of intrinsically disordered proteins induces stepwise target recognition

机译:本质上无序的蛋白质的结构灵活性诱导逐步目标识别。

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An intrinsically disordered protein (IDP) lacks a stable three-dimensional structure, while it folds into a specific structure when it binds to a target molecule. In some IDP-target complexes, not all target binding surfaces are exposed on the outside, and intermediate states are observed in their binding processes. We consider that stepwise target recognition via intermediate states is a characteristic of IDP binding to targets with "hidden" binding sites. To investigate IDP binding to hidden target binding sites, we constructed an IDP lattice model based on the HP model. In our model, the IDP is modeled as a chain and the target is modeled as a highly coarse-grained object. We introduced motion and internal interactions to the target to hide its binding sites. In the case of unhidden binding sites, a two-state transition between the free states and a bound state is observed, and we consider that this represents coupled folding and binding. Introducing hidden binding sites, we found an intermediate bound state in which the IDP forms various structures to temporarily stabilize the complex. The intermediate state provides a scaffold for the IDP to access the hidden binding site. We call this process multiform binding. We conclude that structural flexibility of IDPs enables them to access hidden binding sites and this is a functional advantage of IDPs.
机译:本质上无序的蛋白质(IDP)缺乏稳定的三维结构,但当它与靶分子结合时会折叠成特定的结构。在某些IDP靶复合物中,并非所有靶结合表面都暴露在外面,并且在其结合过程中观察到中间状态。我们认为通过中间状态逐步识别目标是IDP结合具有“隐藏”结合位点的目标的特征。为了研究IDP与隐藏目标结合位点的结合,我们基于HP模型构建了IDP晶格模型。在我们的模型中,将IDP建模为链,将目标建模为高度粗粒度的对象。我们向目标引入了运动和内部相互作用,以隐藏其结合位点。在未隐藏的结合位点的情况下,观察到自由状态和结合状态之间的两个状态的过渡,我们认为这代表了折叠和结合的结合。引入隐藏的结合位点,我们发现了中间结合状态,其中IDP形成各种结构以暂时稳定复合物。中间状态为IDP提供了一个访问隐藏绑定站点的支架。我们称此过程为多格式绑定。我们得出结论,IDP的结构灵活性使它们能够访问隐藏的绑定位点,这是IDP的功能优势。

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