Photoexcited Electro‐Driven Reactive Oxygen Species Channeling for Precise Extraction of Biomarker Information from Tumor Interstitial Fluid

IF 13 2区 材料科学 Q1 CHEMISTRY, MULTIDISCIPLINARY Small Pub Date : 2025-01-07 DOI:10.1002/smll.202410358
Xiyue Xie, Shuqi Tang, Chunhui Zhai, Kaixiu Fu, Fan Li, Kaiyong Cai, Jixi Zhang
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Abstract

Direct electrochemical detection of miRNA biomarkers in tumor tissue interstitial fluid (TIF) holds great promise for adjuvant therapy for tumors in the perioperative period, yet is limited by background interference and weak signal. Herein, a wash‐free and separation‐free miRNA biosensor based on photoexcited electro‐driven reactive oxygen channeling analysis (LEOCA) is developed to solve the high‐fidelity detection in physiological samples. In the presence of miRNA, nanoacceptors (ultrasmall‐size polydopamine, uPDA) are responsively assembled on the surface of nanodonors (zirconium metal‐organic framework, ZrMOF) to form core‐satellite aggregates. The produced lifetime‐constraint singlet oxygen upon light irradiation is captured by the catechol of constrained uPDA, and the oxidized quinone is immediately electro‐reduced to the catechol at transient collision process on the electrode, resulting in a cascade electron transfer and amplified current. Thereby, the nanosensor exhibits a low detection limit (1.1 fM), and high reproducibility (relative standard deviation of 2.0%). Compared with quantitative real‐time polymerase chain reaction (qRT‐PCR), the clinical accuracy (area under the curve value) is significantly increased from 0.75 to 0.93 in distinguishing breast cancer patients from healthy donors. This study demonstrates an inspiration on the synergy of the reactive oxygen channeling between nanodonor/nanoacceptor and the synchronous electron transfer cascade on the electrode to solve the bottleneck problem of detecting unprocessed clinical samples in a sample‐in‐answer‐out manner.
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直接电化学检测肿瘤组织间质(TIF)中的miRNA生物标记物,为围手术期的肿瘤辅助治疗带来了巨大希望,但却受到背景干扰和信号弱的限制。本文开发了一种基于光激发电驱动活性氧通道分析(LEOCA)的免清洗、免分离 miRNA 生物传感器,以解决生理样本中的高保真检测问题。在 miRNA 存在的情况下,纳米受体(超小型多巴胺,uPDA)反应性地组装在纳米载体(锆金属有机框架,ZrMOF)表面,形成核心-卫星聚集体。在光照射下产生的受限寿命的单线态氧被受限 uPDA 的儿茶酚捕获,氧化后的醌在电极上的瞬时碰撞过程中立即被电还原为儿茶酚,从而产生级联电子转移和放大电流。因此,该纳米传感器的检测限低(1.1 fM),重现性高(相对标准偏差为 2.0%)。与实时定量聚合酶链反应(qRT-PCR)相比,在区分乳腺癌患者和健康供体方面,临床准确性(曲线下面积值)从 0.75 显著提高到 0.93。这项研究从纳米载体/纳米受体之间的活性氧通道和电极上的同步电子传递级联的协同作用中得到了启发,从而解决了以 "样本-回答-输出 "方式检测未处理临床样本的瓶颈问题。
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来源期刊
Small
Small 工程技术-材料科学:综合
CiteScore
17.70
自引率
3.80%
发文量
1830
审稿时长
2.1 months
期刊介绍: Small serves as an exceptional platform for both experimental and theoretical studies in fundamental and applied interdisciplinary research at the nano- and microscale. The journal offers a compelling mix of peer-reviewed Research Articles, Reviews, Perspectives, and Comments. With a remarkable 2022 Journal Impact Factor of 13.3 (Journal Citation Reports from Clarivate Analytics, 2023), Small remains among the top multidisciplinary journals, covering a wide range of topics at the interface of materials science, chemistry, physics, engineering, medicine, and biology. Small's readership includes biochemists, biologists, biomedical scientists, chemists, engineers, information technologists, materials scientists, physicists, and theoreticians alike.
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