通过多肽定向自组装构建分层等离子体生物材料的机制

IF 13.9 Q1 CHEMISTRY, MULTIDISCIPLINARY
Lubna Amer, Maurice Retout, Zhicheng Jin, Sumathi Kakanar, Jesse V. Jokerst
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引用次数: 0

摘要

由小纳米颗粒(NPs)组成的分层等离子体生物材料结合成更大的微米级结构,表现出独特的性能,可以用于各种应用。利用扩散限制聚集(DLA)和确定的肽序列,我们开发了具有布朗树结构的分形银生物材料。该方法避免了复杂的氧化还原化学,并可以通过多肽设计和浓度精确控制颗粒间距离和材料形态。我们的系统研究揭示了多肽电荷、长度和序列如何影响生物材料的形态,证实了多肽作为颗粒之间的桥接基序并诱导聚结。通过光谱和显微镜的表征表明,基于精氨酸的肽是基于定量和定性测量的分形组装的最佳选择。此外,我们对扩散行为的研究证实了粒径、温度和介质粘度对纳米颗粒迁移率的影响。这项工作还提供了对银NPs的面分布及其组装机制的见解,为医疗,环境和电子应用的材料设计提供了潜在的进步。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Mechanism of hierarchical plasmonic biomaterials engineered through peptide-directed self-assembly

Mechanism of hierarchical plasmonic biomaterials engineered through peptide-directed self-assembly

Hierarchical plasmonic biomaterials constructed from small nanoparticles (NPs) that combine into larger micron-sized structures exhibit unique properties that can be harnessed for various applications. Using diffusion-limited aggregation (DLA) and defined peptide sequences, we developed fractal silver biomaterials with a Brownian tree structure. This method avoids complex redox chemistry and allows precise control of interparticle distance and material morphology through peptide design and concentration. Our systematic investigation revealed how peptide charge, length, and sequence impact biomaterial morphology, confirming that peptides act as bridging motifs between particles and induce coalescence. Characterization through spectroscopy and microscopy demonstrated that arginine-based peptides are optimal for fractal assembly based on both quantitative and qualitative measurements. Additionally, our study of diffusion behavior confirmed the effect of particle size, temperature, and medium viscosity on nanoparticle mobility. This work also provides insights into the facet distribution in silver NPs and their assembly mechanisms, offering potential advancements in the design of materials for medical, environmental, and electronic applications.

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来源期刊
CiteScore
17.40
自引率
0.00%
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审稿时长
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