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Interplay between desolvation and secondary structure in mediating cosolvent and temperature induced alpha-synuclein aggregation

机译:在介质脱溶剂和温度诱导α-突触核蛋白聚集中的脱溶解与二次结构之间的相互作用

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摘要

Both increased temperature and moderate concentrations of fluorinated alcohols enhance aggregation of the Parkinson’s disease-associated protein α–synuclein (αS). Here, we investigate the secondary structural rearrangements induced by heating and trifluoroethanol (TFE). At low TFE concentrations, CD spectra feature a negative peak characteristic of disordered polypeptides near 200 nm and a slight shoulder around 220 nm suggesting some polyproline-II content. Upon heating, these peaks weaken, while a weak negative signal develops at 222 nm. At high TFE concentrations, the spectra show distinct minima at 208 and 222 nm, indicative of considerable α-helical structure, which diminish upon heating. We observe a crossover between the low-TFE and high-TFE behavior near 15% TFE, where we previously showed that a partially helical intermediate is populated. We postulate that the protein is well solvated by water at low TFE concentrations and by TFE at high TFE concentrations, but may become desolvated at the crossover point. We discuss the potential roles and interplay of desolvation and helical secondary structure in driving αS aggregation.
机译:温度升高和中等浓度的氟化醇均会增强帕金森氏病相关蛋白α–突触核蛋白(αS)的聚集。在这里,我们研究了由加热和三氟乙醇(TFE)引起的二级结构重排。在低TFE浓度下,CD光谱在200 nm附近具有无序多肽的负峰特征,在220 nm附近具有轻微的肩峰,表明某些脯氨酸II含量。加热后,这些峰减弱,而在222 nm处出现弱的负信号。在高TFE浓度下,光谱在208和222 nm处显示出明显的最小值,表明存在明显的α螺旋结构,该结构在加热时会减小。我们观察到在接近15%TFE的情况下,低TFE和高TFE行为之间发生了交叉,在此之前我们表明存在部分螺旋状的中间体。我们假设该蛋白质在低TFE浓度下被水很好地溶解,在高TFE浓度下被TFE很好地溶解,但是在交叉点可能会被去溶剂化。我们讨论了去溶剂化和螺旋二级结构在驱动αS聚集中的潜在作用和相互作用。

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