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β-桶寡聚物作为多肽自组装形成交叉β 聚集物的常见中间体。

β-barrel Oligomers as Common Intermediates of Peptides Self-Assembling into Cross-β Aggregates.

机构信息

Department of Physics and Astronomy, Clemson University, Clemson, SC, 29634, USA.

出版信息

Sci Rep. 2018 Jul 9;8(1):10353. doi: 10.1038/s41598-018-28649-7.

Abstract

Oligomers populated during the early amyloid aggregation process are more toxic than mature fibrils, but pinpointing the exact toxic species among highly dynamic and heterogeneous aggregation intermediates remains a major challenge. β-barrel oligomers, structurally-determined recently for a slow-aggregating peptide derived from αB crystallin, are attractive candidates for exerting amyloid toxicity due to their well-defined structures as therapeutic targets and compatibility to the "amyloid-pore" hypothesis of toxicity. To assess whether β-barrel oligomers are common intermediates to amyloid peptides - a necessary step toward associating β-barrel oligomers with general amyloid cytotoxicity, we computationally studied the oligomerization and fibrillization dynamics of seven well-studied fragments of amyloidogenic proteins with different experimentally-determined aggregation morphologies and cytotoxicity. In our molecular dynamics simulations, β-barrel oligomers were only observed in five peptides self-assembling into the characteristic cross-β aggregates, but not the other two that formed polymorphic β-rich aggregates as reported experimentally. Interestingly, the latter two peptides were previously found nontoxic. Hence, the observed correlation between β-barrel oligomers formation and cytotoxicity supports the hypothesis of β-barrel oligomers as the common toxic intermediates of amyloid aggregation.

摘要

寡聚物在早期淀粉样蛋白聚集过程中更为有毒,比成熟的纤维更具毒性,但在高度动态和异质的聚集中间体中准确确定确切的有毒物质仍然是一个主要挑战。β-桶寡聚物最近因其结构确定而成为具有吸引力的候选物,因为其作为治疗靶点的明确结构和与毒性的“淀粉样蛋白孔”假说的兼容性。为了评估β-桶寡聚物是否是淀粉样肽的常见中间体-将β-桶寡聚物与一般淀粉样细胞毒性相关联的必要步骤,我们通过计算研究了具有不同实验确定的聚集形态和细胞毒性的七种研究良好的淀粉样蛋白片段的寡聚化和纤维化动力学。在我们的分子动力学模拟中,仅在五个自组装成特征性交叉-β聚集体的肽中观察到β-桶寡聚物,而在另外两个如实验中报道的那样形成多态性β-丰富聚集体的肽中则没有观察到。有趣的是,后两种肽以前被发现是无毒的。因此,观察到的β-桶寡聚物形成与细胞毒性之间的相关性支持β-桶寡聚物作为淀粉样蛋白聚集的常见毒性中间体的假说。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2217/6037789/d4b0127e1800/41598_2018_28649_Fig1_HTML.jpg

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