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A Desolvation Model for Trifluoroethanol-Induced Aggregation of Enhanced Green Fluorescent Protein

机译:三氟乙醇诱导的增强型绿色荧光蛋白聚集的去溶剂化模型。

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摘要

Studies of amyloid disease-associated proteins in aqueous solutions containing 2,2,2-trifluoroethanol (TFE) have shown that the formation of structural intermediates is often correlated with enhanced protein aggregation. Here, enhanced green fluorescent protein (EGFP) is used as a model protein system to investigate the causal relationship between TFE-induced structural transitions and aggregation. Using circular dichroism spectroscopy, light scattering measurements, and transmission electron microscopy imaging, we demonstrate that population of a partially α-helical, monomeric intermediate is roughly correlated with the growth of β-sheet-rich, flexible fibrils for acid-denatured EGFP. By fitting our circular dichroism data to a model in which TFE-water mixtures are assumed to be ideal solutions, we show that increasing entropic costs of protein solvation in TFE-water mixtures may both cause the population of the intermediate state and increase aggregate production. Tertiary structure and electrostatic repulsion also impede aggregation. We conclude that initiation of EGFP aggregation in TFE likely involves overcoming of multiple protective factors, rather than stabilization of aggregation-prone structural elements.
机译:在含有2,2,2-三氟乙醇(TFE)的水溶液中与淀粉样蛋白疾病相关的蛋白质的研究表明,结构中间体的形成通常与增强的蛋白质聚集相关。在这里,增强的绿色荧光蛋白(EGFP)被用作模型蛋白系统,以研究TFE诱导的结构转变与聚集之间的因果关系。使用圆二色光谱,光散射测量和透射电子显微镜成像,我们证明了部分α-螺旋的单体中间体的种群与酸性变性EGFP的富含β-折叠的柔性纤维的生长大致相关。通过将我们的圆二色性数据拟合到假设TFE-水混合物是理想解决方案的模型中,我们表明,在TFE-水混合物中增加的蛋白质溶剂化熵成本可能会导致中间状态的发生并增加总产量。三级结构和静电排斥也阻碍聚集。我们得出结论,在TFE中启动EGFP聚集可能涉及克服多种保护因素,而不是稳定易聚集的结构元件。

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