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首页> 外文期刊>Chemical science >Peptidomimetics prepared by tail-to-side chain one component peptide stapling inhibit Alzheimer's amyloid-β fibrillogenesis
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Peptidomimetics prepared by tail-to-side chain one component peptide stapling inhibit Alzheimer's amyloid-β fibrillogenesis

机译:通过尾侧链制备的肽菌肽一组分肽吻合抑制阿尔茨海默蛋白淀粉样蛋白-β原纤维化

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摘要

Alzheimer's disease (AD) is the most common form of dementia affecting the elderly population worldwide. Despite enormous efforts and considerable advancement in research, no therapeutic agents have come to light to date. However, many peptide-based and small molecule inhibitors interact efficiently with the amyloid-β (Aβ) peptide and alter its aggregation pathway. On the other hand, stapled peptides have been developed mainly to stabilize α-helix conformations and study protein–protein interactions. β-Sheet stabilization or destabilization by stapled peptides has not been explored enough. Herein, we describe the generation of a library of “tail-to-side chain” stapled peptides via lactamization and their application for the first time as modulators of Aβ _(1-40) self-association and fibrillogenesis. They also disrupt the preformed fibrillar aggregates into nontoxic species. Their stability in the presence of proteolytic enzymes is increased due to stapling. Therefore, the stapled peptides thus formed can be useful as potent amyloid aggregation inhibitors and pave a therapeutic pathway for combating amyloid-related diseases. Also, they may help in gaining insight into the process of aggregation.
机译:阿尔茨海默病(AD)是影响全世界老年人人口的最常见的痴呆形式。尽管在研究中努力和相当大的进步,但迄今为止没有治疗剂。然而,许多肽基和小分子抑制剂用淀粉样蛋白-β(Aβ)肽有效地相互作用,并改变其聚集途径。另一方面,已经开发出甜食肽,主要用于稳定α-螺旋构象并研究蛋白质 - 蛋白质相互作用。 β-片状稳定或通过甜食肽的稳定化尚未得到足够的。在此,我们描述了通过裂酰胺化的“尾侧链”栓肽的生成及其施用作为Aβ_(1-40)自我关联和纤维发生的调节剂。它们还破坏了预成型的纤维菌聚集体进入无毒物种。由于装订,它们在蛋白水解酶存在下的稳定性增加。因此,由此形成的甜食肽可用作有效的淀粉样蛋白聚集抑制剂并铺平治疗途径以进行淀粉样蛋白相关疾病。此外,他们可能有助于获得洞察聚集过程。

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