首页> 外文期刊>Journal of nanoparticle research: An interdisciplinary forum for nanoscale science and technology >Enhanced antimicrobial activity of silver nanoparticles conjugated with synthetic peptide by click chemistry
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Enhanced antimicrobial activity of silver nanoparticles conjugated with synthetic peptide by click chemistry

机译:通过点击化学增强与合成肽缀合的银纳米粒子的增强抗菌活性

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摘要

Strategies to design novel antibacterial materials may rely on the combination of materials to achieve synergistic effects. The coupling of antibacterial peptides to nanoparticles, however, needs to be directed conveniently to avoid structural changes within the peptide and/or degradation of the nanoparticle. Here, we present the results of the attachment of a synthetic peptide (VIHGW-alkyne-G-NH2) containing the amino terminal copper and nickel (ATCUN) motif to silver nanoparticles. In order to direct the peptide-nanoparticle coupling, the peptide was functionalized with an alkyne, whereas the nanoparticles were functionalized with azide groups using thiol-polyethylene glycol-azide (HS-PEG-N-3) chains, so that the acetylide and the azide can undergo a click reaction. The reaction was conducted at room temperature and the steps in the construction of the nanoparticle-PEG-ATCUN array were followed by a combination of UV-Vis absorption spectroscopy, X-ray photoelectron spectroscopy (XPS), and infrared spectroscopy. Evidence of the attachment of the PEG molecules through the thiol termination indicates that the nanoparticle is functionalized with azide groups, although only partially. The click reaction with the synthetic peptide is evidenced by the loss of the N-3-vibrational signal with infrared spectroscopy. Throughout the steps of the synthesis, the behavior of the nanoparticles was followed by UV-Vis spectroscopy, dynamic light scattering, and zeta potential measurements, observing that during the process there are no significant changes in the size of the nanoparticle and that the stability of the nanoparticles increases. Antibacterial tests, conducted using E. coli, showed that the activity of the Ag-PEG-ATCUN nanocomposites is higher than that of nanoparticles and ATCUN peptides separately.
机译:设计新型抗菌材料的策略可以依赖于材料的组合来实现协同效应。然而,需要方便地引导抗菌肽与纳米颗粒的偶联以避免肽和/或纳米颗粒的降解内的结构变化。这里,我们介绍将含有氨基末端铜和镍(ATCUN)基序与银纳米颗粒的合成肽(Vihgw-alkyne-G-NH2)的附着的结果。为了引导肽纳米粒子偶联,用炔烃官能化肽,而纳米颗粒用硫醇 - 聚乙二醇 - 叠氮化物(HS-PEG-N-3)链用叠氮基团官能化,使乙酰乙烯酯和叠氮化物可以接受点击反应。在室温下进行反应,并在纳米粒子-PEG-ATCUN阵列的构建中进行步骤,然后是UV-Vis吸收光谱,X射线光电子能谱(XPS)和红外光谱的组合。通过硫醇终止将PEG分子连接的证据表明纳米颗粒用叠氮基团官能化,尽管仅部分。通过用红外光谱损失N-3振动信号的损失,可以证明与合成肽的点击反应。在整个合成的步骤中,纳米颗粒的行为之后是UV-Vis光谱,动态光散射和Zeta电位测量,观察到在该过程中纳米粒子的尺寸没有显着变化,并且稳定性纳米颗粒增加。使用大肠杆菌进行的抗菌试验表明,Ag-PEG-ATCUN纳米复合材料的活性分别高于纳米颗粒和ATCUN肽的活性。

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