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基于结构的设计非天然氨基酸抑制剂抑制淀粉样纤维形成。

Structure-based design of non-natural amino-acid inhibitors of amyloid fibril formation.

机构信息

Department of Biological Chemistry, Howard Hughes Medical Institute, UCLA, Box 951970, Los Angeles, California 90095-1570, USA.

出版信息

Nature. 2011 Jun 15;475(7354):96-100. doi: 10.1038/nature10154.

Abstract

Many globular and natively disordered proteins can convert into amyloid fibrils. These fibrils are associated with numerous pathologies as well as with normal cellular functions, and frequently form during protein denaturation. Inhibitors of pathological amyloid fibril formation could be useful in the development of therapeutics, provided that the inhibitors were specific enough to avoid interfering with normal processes. Here we show that computer-aided, structure-based design can yield highly specific peptide inhibitors of amyloid formation. Using known atomic structures of segments of amyloid fibrils as templates, we have designed and characterized an all-D-amino-acid inhibitor of the fibril formation of the tau protein associated with Alzheimer's disease, and a non-natural L-amino-acid inhibitor of an amyloid fibril that enhances sexual transmission of human immunodeficiency virus. Our results indicate that peptides from structure-based designs can disrupt the fibril formation of full-length proteins, including those, such as tau protein, that lack fully ordered native structures. Because the inhibiting peptides have been designed on structures of dual-β-sheet 'steric zippers', the successful inhibition of amyloid fibril formation strengthens the hypothesis that amyloid spines contain steric zippers.

摘要

许多球状和天然无规的蛋白质可以转化为淀粉样纤维。这些纤维与许多病理以及正常的细胞功能有关,并且经常在蛋白质变性过程中形成。病理性淀粉样纤维形成的抑制剂在治疗学的发展中可能是有用的,只要抑制剂足够特异以避免干扰正常过程。在这里,我们展示了计算机辅助的基于结构的设计可以产生淀粉样形成的高度特异的肽抑制剂。使用淀粉样纤维片段的已知原子结构作为模板,我们设计并表征了一种与阿尔茨海默病相关的 tau 蛋白纤维形成的全 D-氨基酸抑制剂,以及一种增强人类免疫缺陷病毒性传播的淀粉样纤维的非天然 L-氨基酸抑制剂。我们的结果表明,基于结构设计的肽可以破坏全长蛋白质的纤维形成,包括那些缺乏完全有序的天然结构的蛋白质,如 tau 蛋白。由于抑制肽是根据双β-折叠“空间拉链”的结构设计的,淀粉样纤维形成的成功抑制加强了淀粉样纤维包含空间拉链的假说。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dfe5/4073670/709836ac20dd/nihms591364f1.jpg

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