Extended Spherical Diffusion Theory: Electrochemiluminescence Imaging Analysis of Diffusive Molecules from Spherical Biosamples.

IF 6.7 1区 化学 Q1 CHEMISTRY, ANALYTICAL Analytical Chemistry Pub Date : 2024-11-18 DOI:10.1021/acs.analchem.4c03167
Kosuke Ino, Miyu Mashiko, Yusuke Kanno, Yeyi Tang, Shuzo Masui, Takasi Nisisako, Kaoru Hiramoto, Hiroya Abe, Hitoshi Shiku
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Abstract

Spherical biosamples such as immunobeads, cells, and cell aggregates have been widely used in bioapplications. The bioactivity of individual spherical biosamples in highly sensitive assays and individual analyses must be evaluated in a high-throughput manner. Electrochemiluminescence (ECL) imaging was recently proposed for the high-throughput analysis of diffusive molecules from spherical biosamples. ECL imaging involves the placing of spherical biosamples on a flat electrode filled with a solution. The biosamples produce (or consume) biological/chemical molecules such as H2O2 and O2, which diffuse to form a concentration gradient at the electrode. The ECL signals from the molecules are then measured to obtain the concentration profile, which allows the flux to be estimated, from which their bioactivities can be successfully calculated. However, no studies on theoretical approaches for spherical biosamples on flat surfaces have been conducted using ECL imaging. Therefore, this paper presents a novel spherical diffusion theory for spherical biosamples on a flat surface, which is based on the common spherical diffusion theory and was designated as the extended spherical diffusion theory. First, the concepts behind this theory are discussed. The theory is then validated by comparison with a simulated analysis. The resulting equation successfully expresses the concentration profile for the entire area. The glucose oxidase activity in the hydrogel beads is subsequently visualized using ECL imaging, and the enzymatic product flux is calculated using the proof-of-concept theory. Finally, a time-dependent simulation is conducted to fill the gap between the theoretical and experimental data. This paper presents novel guidelines for this analysis.

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扩展球形扩散理论:球形生物样品中扩散分子的电化学发光成像分析。
球形生物样品(如免疫球蛋白、细胞和细胞聚集体)已被广泛用于生物应用中。在高灵敏度检测和单项分析中,必须以高通量方式评估单个球形生物样品的生物活性。最近,有人提出用电化学发光(ECL)成像技术对球形生物样品中的扩散分子进行高通量分析。ECL 成像技术是将球形生物样品置于充满溶液的平面电极上。生物样品产生(或消耗)H2O2 和 O2 等生物/化学分子,这些分子扩散后在电极上形成浓度梯度。然后测量来自分子的 ECL 信号,以获得浓度曲线,从而估算通量,并据此成功计算出其生物活性。然而,目前还没有利用 ECL 成像对平面上的球形生物样品进行理论研究。因此,本文在普通球形扩散理论的基础上,提出了一种适用于平面上球形生物样品的新型球形扩散理论,并将其命名为扩展球形扩散理论。首先,讨论了该理论背后的概念。然后,通过与模拟分析的对比验证了该理论。由此得出的方程成功地表达了整个区域的浓度曲线。随后,利用 ECL 成像对水凝胶珠中的葡萄糖氧化酶活性进行了可视化,并利用概念验证理论计算了酶产物通量。最后,进行了随时间变化的模拟,以填补理论数据与实验数据之间的差距。本文为这一分析提出了新的指导原则。
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来源期刊
Analytical Chemistry
Analytical Chemistry 化学-分析化学
CiteScore
12.10
自引率
12.20%
发文量
1949
审稿时长
1.4 months
期刊介绍: Analytical Chemistry, a peer-reviewed research journal, focuses on disseminating new and original knowledge across all branches of analytical chemistry. Fundamental articles may explore general principles of chemical measurement science and need not directly address existing or potential analytical methodology. They can be entirely theoretical or report experimental results. Contributions may cover various phases of analytical operations, including sampling, bioanalysis, electrochemistry, mass spectrometry, microscale and nanoscale systems, environmental analysis, separations, spectroscopy, chemical reactions and selectivity, instrumentation, imaging, surface analysis, and data processing. Papers discussing known analytical methods should present a significant, original application of the method, a notable improvement, or results on an important analyte.
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