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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Nanofibrous scaffold from self-assembly of β-sheet peptides containing phenylalanine for controlled release
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Nanofibrous scaffold from self-assembly of β-sheet peptides containing phenylalanine for controlled release

机译:自组装含苯丙氨酸的β-折叠肽的自组装纳米纤维支架,用于控释

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摘要

Scaffold nanostructures from self-assembly of β-sheet peptides, RADAFI and RADAFII, containing same amino acid compositions but different positions of one phenylalanine residue, were investigated. Atomic force microscopy (AFM) images clearly showed that peptide RADAFI self-assembled into twisted nanofibers with multiple molecular sized width and height, but no twisted nanofiber, characterized by a stacked bilayer model with single molecular sized width, was obtained in RADAFII scaffold. Two models of the hierarchical self-assembling behaviors could be illustrated for RADAFI and RADAFII scaffolds. The peptide scaffolds might also be promising for a variety of possible biomedical applications, including drug delivery, and the results revealed some relationships among the peptide sequence, the network nanoarchitecture, and the controlled release. From the remarkably large difference between the architecture and properties of the self-assembling materials based on the two similar peptides, it could be concluded that the self-assembly behaviors were delicate and could be dramatically altered by small modifying peptide structural features due to subtle changing the phenyl group position. The presence of a center π–π stacking between two β-sheet-forming strands in the peptide sequence was demonstrated to be an important factor in promoting the twisted nanofiber morphology and a stronger network. Also, the concept of dominating the network nanostructures could be harnessed in the de novo design of delivery materials for some special biomolecules
机译:研究了β-折叠肽自组装的支架纳米结构,RADAFI和RADAFII,其氨基酸组成相同,但一个苯丙氨酸残基的位置不同。原子力显微镜(AFM)图像清楚地显示,在RADAFII支架中,多肽RADAFI自组装成具有多个分子大小的宽度和高度的扭曲纳米纤维,但没有扭曲纳米纤维,其特征在于具有单个分子大小宽度的堆叠双层模型。可以为RADAFI和RADAFII脚手架说明分层自组装行为的两个模型。肽支架可能还有望用于包括药物递送在内的多种可能的生物医学应用中,结果揭示了肽序列,网络纳米结构和控释之间的某些关系。从基于两种相似肽的自组装材料的结构和性能之间的巨大差异来看,可以得出结论,自组装行为是微妙的,并且由于细微变化而被小的修饰肽结构特征所改变,可以大大改变自组装行为苯基位置。肽序列中两个形成β-折叠的链之间存在中心π-π堆积被证明是促进扭曲的纳米纤维形态和更牢固网络的重要因素。同样,支配网络纳米结构的概念可以在从头设计某些特殊生物分子的输送材料时采用

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