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具有工程化 GE11 肽的等离子体纳米结构增强的 EGFR 靶向活性。

Enhanced EGFR Targeting Activity of Plasmonic Nanostructures with Engineered GE11 Peptide.

机构信息

Department of Chemical Sciences, University of Padova, Via Marzolo 1, 35131, Padova, Italy.

Department of Surgery Oncology and Gastroenterology, University of Padova, Via Giustiniani, 2, 35124, Padova, Italy.

出版信息

Adv Healthc Mater. 2017 Dec;6(23). doi: 10.1002/adhm.201700596. Epub 2017 Sep 25.

DOI:10.1002/adhm.201700596
PMID:28945012
Abstract

Plasmonic nanostructures show important properties for biotechnological applications, but they have to be guided on the target for exploiting their potentialities. Antibodies are the natural molecules for targeting. However, their possible adverse immunogenic activity and their cost have suggested finding other valid substitutes. Small molecules like peptides can be an alternative source of targeting agents, even if, as single molecules, their binding affinity is usually not very good. GE11 is a small dodecapeptide with specific binding to the epidermal growth factor receptor (EGFR) and low immunogenicity. The present work shows that thousands of polyethylene glycol (PEG) chains modified with lysines and functionalized with GE11 on clusters of naked gold nanoparticles, obtained by laser ablation in water, achieves a better targeting activity than that recorded with nanoparticles decorated with the specific anti-EGFR antibody Cetuximab (C225). The insertion of the cationic spacer between the polymeric part of the ligand and the targeting peptide allows for a proper presentation of GE11 on the surface of the nanosystems. Surface enhanced resonance Raman scattering signals of the plasmonic gold nanoparticles are used for quantifying the targeting activity. Molecular dynamic calculations suggest that subtle differences in the exposition of the peptide on the PEG sea are important for the targeting activity.

摘要

等离子体纳米结构在生物技术应用中表现出重要的性质,但为了发挥其潜力,它们必须被引导到目标上。抗体是靶向的天然分子。然而,它们可能的免疫原性和成本促使人们寻找其他有效的替代品。小分子如肽可以作为靶向试剂的替代来源,即使作为单个分子,它们的结合亲和力通常不是很好。GE11 是一种具有特异性结合表皮生长因子受体(EGFR)和低免疫原性的十二肽。本工作表明,在裸金纳米粒子簇上用赖氨酸修饰并通过激光烧蚀在水中功能化的数千个聚乙二醇(PEG)链,比用特异性抗 EGFR 抗体 Cetuximab(C225)修饰的纳米粒子记录的靶向活性更好。将配体的聚合物部分和靶向肽之间的阳离子间隔物插入,可使 GE11 在纳米系统表面上适当呈现。等离子体金纳米粒子的表面增强共振拉曼散射信号用于定量靶向活性。分子动力学计算表明,肽在 PEG 海洋上的暴露的细微差异对靶向活性很重要。

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