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Entropic Control of an Excited Folded-Like Conformation in a Disordered Protein Ensemble

机译:混乱的蛋白质组合中的兴奋折叠样构象的熵控制。

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摘要

Many intrinsically disordered proteins switch between unfolded and folded-like forms in the presence of their binding partner. The possibility of a pre-equilibrium between the two macrostates is challenging to discern given the complex conformational landscape. Here, we show that CytR, a disordered DNA-binding domain, samples a folded-like excited state in its native ensemble through equilibrium multi-probe spectroscopy, kinetics and an Ising-like statistical mechanical model. The population of the excited state increases upon stabilization of the native ensemble with an osmolyte, while decreasing with increasing temperatures. A conserved proline residue, the mutation of which weakens the binding affinity to the target promoter, is found to uniquely control the population of the minor excited state. Semi-quantitative statistical mechanical modeling reveals that the conformational diffusion coefficient of disordered CytR is an order of magnitude slower than the estimates from folded domains. The osmolyte and proline mutation smoothen and roughen up the landscape, respectively, apart from modulation of populations. Our work uncovers general strategies to probe for excited structured states in disordered ensembles, and to measure and modulate the roughness of the disordered landscapes, inter-conversion rates of species and their populations.
机译:在结合伴侣的存在下,许多内在无序的蛋白质在未折叠和折叠样形式之间切换。考虑到复杂的构象态势,要辨别两个大状态之间的预平衡的可能性是具有挑战性的。在这里,我们显示CytR,一个无序的DNA结合结构域,通过平衡多探针光谱,动力学和类似于Ising的统计力学模型,在其天然集合中采样了折叠状的激发态。激发态的种群随着渗透液的稳定而增加,而随着温度的升高而减少。发现保守的脯氨酸残基,其突变削弱了对靶启动子的结合亲和力,其独特地控制了次要激发态的总体。半定量统计力学建模表明,无序CytR的构象扩散系数比折叠域的估计慢一个数量级。除了调节种群外,渗透压和脯氨酸突变分别使景观变得平滑和粗糙。我们的工作揭示了探索无序合奏中激发结构状态的常规策略,并测量和调节无序景观的粗糙度,物种及其种群的相互转化率。

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