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Multi-Domain Short Peptide Molecules for in Situ Synthesis and Biofunctionalization of Gold Nanoparticles for Integrin-Targeted Cell Uptake

机译:多域短肽分子用于原位合成和生物功能化金纳米颗粒的整合素靶向细胞摄取。

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摘要

We describe design and synthesis model of multidomain (modular) peptides (MDPs), which direct a reaction cascade coupling the synthesis and surface functionalization of gold nanoparticles (AuNPs) in a single step. The synthesis is achieved via simple mixing of the aqueous solutions of auric acid and MDPs at room temperature without the addition of any surfactants or toxic intermediate reagents. This method allows facile control over the nanoparticle size between ∼2-15 nm, which opens a practical window for biomedical applications. In contrast to the conventional citrate-mediated methods, peptide-mediated synthesis and stabilization provide increased colloidal stability to AuNPs. As a proof of this concept, we demonstrate active targeting of human breast adenocarcinoma cell line (MCF7) using the one-step-prepared engineered AuNPs. Overall, we propose a single-step, chemically greener, biologically safer method for the synthesis and surface functionalization of gold nanoparticles in a size-controlled manner. The chemical versatility of the MDP design broadens the applicability of this strategy, thereby emerging as a successful alternative for the currently available nanoparticle preparation technologies. (Chemical Presented). © 2015 American Chemical Society.
机译:我们描述了多域(模块化)肽(MDPs)的设计和合成模型,该模型指导反应级联在单个步骤中耦合金纳米颗粒(AuNPs)的合成和表面功能化。合成是通过在室温下简单混合金酸和MDP的水溶液而无需添加任何表面活性剂或有毒中间试剂来实现的。这种方法可以轻松控制约2-15 nm之间的纳米颗粒大小,这为生物医学应用打开了实用的窗口。与常规柠檬酸盐介导的方法相反,肽介导的合成和稳定化为AuNPs提供了增加的胶体稳定性。作为该概念的证明,我们证明了使用一步制备的工程化AuNPs主动靶向人乳腺癌细胞系(MCF7)。总体而言,我们提出了一种单步,化学环保,生物安全的方法,用于以尺寸控制的方式合成金纳米颗粒和对其进行表面功能化。 MDP设计的化学多功能性拓宽​​了该策略的适用范围,从而成为当前可用的纳米颗粒制备技术的成功替代方案。 (化学介绍)。 ©2015美国化学学会。

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