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朊病毒肽聚集体中形态、β-折叠稳定性与分子结构之间的相关性。

Correlations among morphology, beta-sheet stability, and molecular structure in prion peptide aggregates.

作者信息

Petty Sarah A, Adalsteinsson Thorsteinn, Decatur Sean M

机构信息

Department of Chemistry, Mount Holyoke College, 50 College Street, South Hadley, Massachusetts 01075, USA.

出版信息

Biochemistry. 2005 Mar 29;44(12):4720-6. doi: 10.1021/bi047445a.

Abstract

The misfolding of proteins into beta-sheets and the subsequent aggregation of these sheets into fibrous networks underlies many diseases. In this paper, the role of peptide structure in determining the ordering of beta-sheet aggregates and the morphology of fibrils and protofibrils is dissected. Using a series of peptides based on residues 109-122 of the Syrian hamster prion protein (H1) with a range of substitutions at position 117, the link between side chain interactions and beta-sheet thermal stability has been investigated. The thermal stability of beta-sheets is associated with the peptides' ability to adopt the same alignment as wild-type H1, with residue 117 in register across all beta-strands [Silva, R. A. G. D., Barber-Armstrong, W., and Decatur, S. M. (2003) J. Am. Chem. Soc. 125, 13674-13675]. These aligned strands are capable of forming long, rigid, and twisted fibrils (as visualized by atomic force microscopy) which are thermostable. Peptides which do not adopt this strand alignment aggregate to form thin, flexible, and smooth protofibrils. The ability to form ordered aggregates, and thus to form twisted fibrils, is modulated by the structure of the side chain of residue 117.

摘要

蛋白质错误折叠成β-折叠片,随后这些折叠片聚集成纤维状网络是许多疾病的根源。在本文中,剖析了肽结构在决定β-折叠聚集体的排列以及原纤维和纤维原纤维形态方面的作用。使用一系列基于叙利亚仓鼠朊病毒蛋白(H1)第109 - 122位残基的肽,在第117位有一系列取代,研究了侧链相互作用与β-折叠热稳定性之间的联系。β-折叠的热稳定性与肽采用与野生型H1相同排列的能力相关,第117位残基在所有β-链中对齐[席尔瓦,R. A. G. D.,巴伯 - 阿姆斯特朗,W.,和迪凯特,S. M.(2003年)《美国化学会志》125,13674 - 13675]。这些对齐的链能够形成长的、刚性的和扭曲的纤维(通过原子力显微镜观察),它们是热稳定的。不采用这种链对齐方式的肽聚集形成薄的、柔性的和平滑的原纤维。形成有序聚集体从而形成扭曲纤维的能力受第117位残基侧链结构的调节。

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