Molecular Engineering of a Doubly Quenched Fluorescent Probe Enables Ultrasensitive Detection of Biothiols in Highly Diluted Plasma and High-Fidelity Imaging of Dihydroartemisinin-Induced Ferroptosis.

IF 6.7 1区 化学 Q1 CHEMISTRY, ANALYTICAL Analytical Chemistry Pub Date : 2024-08-13 Epub Date: 2024-08-01 DOI:10.1021/acs.analchem.4c02431
Qin Zeng, Zhiyang Yuwen, Lemeng Zhang, Yuning Li, Hongwen Liu, Kai Zhang
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Abstract

The occurrence and development of diseases are accompanied by abnormal activity or concentration of biomarkers in cells, tissues, and blood. However, the insufficient sensitivity and accuracy of the available fluorescence probes hinder the precise monitoring of associated indexes in biological systems, which is generally due to the high probe intrinsic fluorescence and false-negative signal caused by the reactive oxygen species (ROS)-induced probe decomposition. To resolve these problems, we have engineered a ROS-stable, meso-carboxylate boron dipyrromethene (BODIPY)-based fluorescent probe, which displays quite a low background fluorescence due to the doubly quenched intrinsic fluorescence by a combined strategy of the photoinduced electron transfer (PET) effect and "ester-to-carboxylate" conversion. The probe achieved a high S/N ratio with ultrasensitivity and good selectivity toward biothiols, endowing its fast detection capability toward the biothiol level in 200×-diluted plasma samples. Using this probe, we achieved remarkable distinguishing of liver injury plasma from normal plasma even at 80× dilution. Moreover, owing to its good stability toward ROS, the probe was successfully employed for high-fidelity imaging of the negative fluctuation of the biothiol level in nonsmall-cell lung cancer (NSCLC) during dihydroartemisinin-induced ferroptosis. This delicate design of suppressing intrinsic fluorescence reveals insights into enhancing the sensitivity and accuracy of fluorescent probes toward the detection and imaging of biomarkers in the occurrence and development of diseases.

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双淬灭荧光探针的分子工程技术实现了高稀释血浆中生物硫醇的超灵敏检测和双氢青蒿素诱导铁中毒的高保真成像。
疾病的发生和发展伴随着细胞、组织和血液中生物标志物的异常活性或浓度。然而,现有荧光探针的灵敏度和准确性不足,阻碍了对生物系统中相关指标的精确监测,这通常是由于探针本征荧光较高,以及活性氧(ROS)诱导探针分解造成的假阴性信号。为了解决这些问题,我们设计了一种 ROS 稳定的介羧酸二吡咯烷硼(BODIPY)基荧光探针,通过光诱导电子转移(PET)效应和 "酯-羧酸 "转换的组合策略,该探针因双重淬灭本征荧光而显示出相当低的背景荧光。该探针具有高信噪比、超灵敏度和对生物硫醇的良好选择性,因此能够快速检测 200 倍稀释血浆样品中的生物硫醇水平。使用该探针,即使在 80 倍稀释的情况下,我们也能明显区分肝损伤血浆和正常血浆。此外,由于该探针对 ROS 具有良好的稳定性,我们还成功地将其用于非小细胞肺癌(NSCLC)在双氢青蒿素诱导铁中毒过程中生物硫醇水平负向波动的高保真成像。这种抑制本征荧光的精巧设计揭示了如何提高荧光探针的灵敏度和准确性,以便对疾病发生和发展过程中的生物标记物进行检测和成像。
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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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