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Insulin and Polylysine as Model Polypeptides for FTI1 Studies of the Pressure-effect on Protein Aggregation

机译:胰岛素和聚赖氨酸作为模型多肽,用于FTI1对蛋白质聚集的压力效应的研究

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High pressure second derivative FTIR spectroscopy has been employed in order to investigate subtle differences between insulin aggregates obtained after 1,2,3,4 , and 5 hours of incubation at 70°C and pD = 2 This study shows that, although the prolonged heating of insulin does result in the increasing content of pressure-insensitive amyloid fibrils, the pressure-sensitive fraction is still present even after long heating of the sample. This suggests that in the inter-fibrillar spaces, small dissociation-prone aggregates are entrapped. High pressure up to approx. 600 MPa acted as if it were capable of partial reversing of the very late stages of the insulin fibrilization. Interestingly, for all the samples examined, pressure increasing up to 1 GPa would not result in further spectral changes. On the other hand, even pressure as low as 30 MPa has been shown to prevent completely aggregation of insulin. Studying heat- and pressure-induced spectral shifts of the amide F band of polylysine in antiparallel β-sheet conformation, the causative role of changing hydration has been implicated. Likewise, a pressure-induced hy-dration of the amyloid may explain the spectral changes occurring upon pressurization of the insulin fibrils.
机译:高压二阶导数FTIR光谱已经为了在70℃和Pd = 2至调查1,2,3,4-之后获得的聚集体的胰岛素,并孵育5小时之间的细微差别这项研究表明采用的是,尽管长时间加热的胰岛素确实在压力不敏感的淀粉样蛋白原纤维的含量的增加结果,压敏馏分甚至在样品的长的加热后仍然存在。这表明,在帧间纤维状空间,小离解倾向聚集体截留。高压高达约600兆帕的举动就好像它是能够扭转部分胰岛素fibrilization的阶段很晚的。有趣的是,对于所有样品检测,压力提高到1GPa的不会导致进一步的光谱变化。在另一方面,即使压力低至30兆帕已显示防止胰岛素完全聚合。研究热和在反向平行的β片层构象的多聚赖氨酸的酰胺˚F带的压力引起的光谱移动,改变水合的致病作用已牵涉。同样地,淀粉样蛋白的压力诱导HY-dration可以解释在所述胰岛素原纤维的加压产生的光谱变化。

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