A novel particle mass calibration strategy for the quantification of AuNPs in single cancer cells via laser ablation ICP-mass spectrometry. A case study

IF 3.1 2区 化学 Q2 CHEMISTRY, ANALYTICAL
Antonio Bazo, Eduardo Bolea-Fernandez, Kharmen Billimoria, Ana Rua-Ibarz, Maite Aramendía, Paula Menero-Valdés, Jack Morley, Sara Neves, Armando Sánchez-Cachero, Heidi Goenaga-Infante and Martín Resano
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Abstract

Laser ablation ICP-mass spectrometry (LA-ICP-MS) has developed as a powerful tool for elemental quantitative analysis of individual cells, assuring that the content of each cell is analyzed individually. However, this technique is still limited by the difficulties associated with calibration using solid standards. This work proposes a particle mass calibration strategy that is independent of both the properties and thickness of the gelatin films used for calibration, overcoming a significant drawback of previously established methods. The fundamental principle of this strategy relies on the individual ablation of nanoparticles (NPs) of well-characterized size that are embedded in the films, so that their mass can be directly used for calibration without the need to calculate their exact concentration within the gelatin. The performance of the newly developed method was compared to that of the previously reported approaches (ionic and particle number calibration) in terms of linearity and homogeneity between different films prepared from the same gelatin solution. As a case study, the three calibration strategies were used for the quantitative analysis of HeLa cancer cells exposed to AuNPs. In parallel, in-suspension single-cell (SC) ICP-MS Au data were obtained and used as reference for comparison with the three LA-SC-ICP-MS strategies. The results obtained with the novel particle mass approach demonstrated better accuracy and repeatability over three different working sessions, addressing key limitations and providing a robust and reliable method for quantitative LA-SC-ICP-MS analysis. The particle mass method holds promise for quantitative LA-ICP-MS analysis of samples beyond NP-exposed cells, such as biological tissues.

Abstract Image

一种新的粒子质量校准策略,用于通过激光烧蚀icp -质谱法定量单个癌细胞中的AuNPs。案例研究
激光烧蚀icp -质谱(LA-ICP-MS)已发展成为单个细胞元素定量分析的强大工具,确保每个细胞的含量被单独分析。然而,这种技术仍然受到使用固体标准进行校准的困难的限制。这项工作提出了一种粒子质量校准策略,该策略独立于用于校准的明胶薄膜的性质和厚度,克服了以前建立的方法的重大缺点。该策略的基本原理依赖于嵌入在薄膜中的具有良好表征尺寸的纳米颗粒(NPs)的单个消融,因此它们的质量可以直接用于校准,而无需计算它们在明胶中的确切浓度。在同一明胶溶液制备的不同薄膜之间的线性和均匀性方面,将新开发的方法与先前报道的方法(离子和粒子数校准)进行了比较。作为一个案例研究,这三种校准策略被用于暴露于aunp的HeLa癌细胞的定量分析。同时,获得悬浮中单细胞(SC) ICP-MS Au数据,并将其作为参考,与三种LA-SC-ICP-MS策略进行比较。在三个不同的工作过程中,新型粒子质量方法获得的结果显示出更好的准确性和可重复性,解决了关键的局限性,并为定量LA-SC-ICP-MS分析提供了一种强大可靠的方法。粒子质量法有望对除np暴露细胞外的样品(如生物组织)进行定量LA-ICP-MS分析。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
6.20
自引率
26.50%
发文量
228
审稿时长
1.7 months
期刊介绍: Innovative research on the fundamental theory and application of spectrometric techniques.
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