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通过引入二级结构构象约束来调整纳米结构肽膜的形态:以分级自组装为例。

Tuning the Morphology of Nanostructured Peptide Films by the Introduction of a Secondary Structure Conformational Constraint: A Case Study of Hierarchical Self-Assembly.

机构信息

Department of Chemistry , University of Padova , Via Marzolo 1 , 35131 Padova , Italy.

Department of Chemical Science and Technologies , University of Rome "Tor Vergata" , Via della Ricerca Scientifica 1 , 00133 Rome , Italy.

出版信息

J Phys Chem B. 2018 Jun 21;122(24):6305-6313. doi: 10.1021/acs.jpcb.8b01877. Epub 2018 Jun 7.

Abstract

Peptide self-assembly is ubiquitous in nature. It governs the organization of proteins, controlling their folding kinetics and preserving their structural stability and bioactivity. In this connection, model oligopeptides may give important insights into the molecular mechanisms and elementary forces driving the formation of supramolecular structures. In this contribution, we show that a single residue substitution, that is, Aib (α-aminoisobutyric acid) in place of Ala at position 4 of an -(l-Ala)-homo-oligomer, strongly alters the aggregation process. In particular, this process is initiated by the formation of small peptide clusters that promote aggregation on the nanometer scale and, through a hierarchical self-assembly, lead to mesoscopic structures of micrometric dimensions. Furthermore, we show that the use of the well-established Langmuir-Blodgett technique represents an effective strategy for coating extended areas of inorganic substrates by densely packed peptide layers, thus paving the way for application of peptide films as templates for biomineralization, biocompatible coating of surfaces, and scaffolds for tissue engineering.

摘要

肽自组装在自然界中无处不在。它控制着蛋白质的组织,控制它们的折叠动力学,并保持它们的结构稳定性和生物活性。在这方面,模型寡肽可以为驱动超分子结构形成的分子机制和基本力提供重要的见解。在本研究中,我们发现,单个残基取代,即在位置 4 用 α-氨基异丁酸(Aib)取代丙氨酸,会强烈改变聚合过程。特别是,该过程由小肽簇的形成引发,小肽簇在纳米尺度上促进聚集,并通过分级自组装形成具有微米尺寸的介观结构。此外,我们还表明,采用成熟的 Langmuir-Blodgett 技术是在无机基底上涂覆密集肽层的有效策略,从而为肽膜作为生物矿化模板、表面生物相容性涂层和组织工程支架铺平了道路。

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