Effect of Surface Modification of Gold Nanoparticles Loaded with Small Nucleic Acid Sequences on Cytotoxicity and Uptake: A Comparative Study In Vitro.

IF 4.7 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2025-04-21 Epub Date: 2025-03-16 DOI:10.1021/acsabm.4c01861
Thuy Truong An Nguyen, Raphaël Dutour, Louise Conrard, Marjorie Vermeersch, Manon Mirgaux, David Perez-Morga, Nicolas Baeyens, Gilles Bruylants, Isabelle Demeestere
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Abstract

Nanoparticle technology, particularly gold nanoparticles (AuNPs), is being developed for a wide range of applications, including as a delivery system of peptides or nucleic acids (NA). Their use in precision medicine requires detailed engineering of NP functionalization to optimize their function and minimize off-target toxicity. Two main routes can be found in the literature for the attachment of NA strands to AuNPs: covalent binding via a thiol group or passive adsorption onto a specially adapted coating previously applied to the metallic core. In this latter case, the coating is often a positively charged polymer, as polyethylenimine, which due to its high positive charge can induce cytotoxicity. Here, we investigated an innovative strategy based on the initial coating of the particles using calix[4]arene macrocycles bearing polyethylene glycol chains as an interesting alternative to polyethylenimine for NA adsorption. Because any molecular modification of AuNPs may affect the cytotoxicity and cellular uptake, we compared the behavior of these AuNPs to that of particles obtained via a classical thiol covalent attachment in MCF-7 and GC-1 spg cell lines. We showed a high biocompatibility of both AuNPs-NA internalized in vitro. The difference in subcellular localization of both AuNPs-NA in MCF-7 cells compared to GC-1 spg cells suggests that their subcellular target is cell- and coating-dependent. This finding provides valuable insights for developing alternative NA delivery systems with a high degree of tunability.

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负载小核酸序列的金纳米颗粒表面修饰对细胞毒性和摄取的影响:体外比较研究。
纳米颗粒技术,特别是金纳米颗粒(AuNPs),正在被开发用于广泛的应用,包括作为肽或核酸(NA)的递送系统。它们在精密医学中的应用需要详细的NP功能化工程,以优化其功能并最大限度地减少脱靶毒性。在文献中可以找到NA链附着到AuNPs上的两种主要途径:通过巯基的共价结合或被动吸附到先前应用于金属核心的特殊适应涂层上。在后一种情况下,涂层通常是带正电荷的聚合物,如聚乙烯亚胺,由于其高正电荷可以诱导细胞毒性。在这里,我们研究了一种创新的策略,该策略基于带有聚乙二醇链的杯状[4]芳烃大环的颗粒初始涂层,作为聚乙烯亚胺吸附NA的有趣替代品。由于AuNPs的任何分子修饰都可能影响细胞毒性和细胞摄取,我们将这些AuNPs的行为与MCF-7和GC-1 spg细胞系中通过经典硫醇共价附着获得的颗粒的行为进行了比较。我们发现这两种AuNPs-NA体外内化具有很高的生物相容性。与GC-1 spg细胞相比,MCF-7细胞中AuNPs-NA的亚细胞定位差异表明,它们的亚细胞靶标依赖于细胞和涂层。这一发现为开发具有高度可调性的替代NA输送系统提供了有价值的见解。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
期刊介绍: ACS Applied Bio Materials is an interdisciplinary journal publishing original research covering all aspects of biomaterials and biointerfaces including and beyond the traditional biosensing, biomedical and therapeutic applications. The journal is devoted to reports of new and original experimental and theoretical research of an applied nature that integrates knowledge in the areas of materials, engineering, physics, bioscience, and chemistry into important bio applications. The journal is specifically interested in work that addresses the relationship between structure and function and assesses the stability and degradation of materials under relevant environmental and biological conditions.
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