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一体化纳米耀斑生物传感器结合催化发夹组装扩增用于原位和灵敏的外泌体微小RNA检测及癌症分类。

All-in-one nanoflare biosensor combined with catalyzed hairpin assembly amplification for in situ and sensitive exosomal miRNA detection and cancer classification.

作者信息

Zhang Xue-Wei, Du Li, Liu Meng-Xian, Wang Jian-Hua, Chen Shuai, Yu Yong-Liang

机构信息

Research Center for Analytical Sciences, Department of Chemistry, College of Sciences, Northeastern University, Shenyang, 110819, China.

Department of Pharmacy, Shanxi Provincial Cancer Hospital, Taiyuan, 110819, China.

出版信息

Talanta. 2024 Jan 1;266(Pt 2):125145. doi: 10.1016/j.talanta.2023.125145. Epub 2023 Aug 31.

Abstract

Exosomal miRNAs can reflect tumor progression and metastasis, and are effective biomarkers for cancer diagnosis. However, the accuracy of exosomal miRNA-based cancer diagnosis is limited by the low sensitivity and complicated RNA extraction of traditional approaches. Herein, a novel biosensor is developed for in situ, extraction-free, and highly sensitive analysis of exosomal miRNAs via nanoflare combined with catalyzed hairpin assembly (CHA) amplification. Without cumbersome and costly miRNA extraction or transfection agents, nanoflare can directly enter the exosomes to bind target miRNAs and generate a fluorescence signal that can be amplified by the CHA reaction to achieve the in situ and highly sensitive detection of exosomal miRNAs. Under the optimal conditions, the detection limit of 5 aM is obtained for three exosomal miRNAs, which is an order of magnitude lower than quantitative real time polymerase chain reaction (qRT-PCR). In combination with the linear discriminant analysis algorithm, five exosomes are distinguished with 100% accuracy. Importantly, five cancers including breast, lung, liver, cervical, and colon cancer from 64 patients are distinguished with 99% accuracy by testing exosomal miRNAs in clinical plasma. This simple, accurate, and sensitive biosensor holds the potential to be expanded into clinical non-invasive cancer diagnostic tests.

摘要

外泌体微小RNA(miRNA)能够反映肿瘤进展和转移情况,是癌症诊断的有效生物标志物。然而,基于外泌体miRNA的癌症诊断准确性受到传统方法低灵敏度和复杂RNA提取过程的限制。在此,通过纳米耀斑与催化发夹组装(CHA)扩增相结合,开发了一种新型生物传感器,用于外泌体miRNA的原位、免提取且高灵敏度分析。无需繁琐且昂贵的miRNA提取或转染试剂,纳米耀斑可直接进入外泌体与靶标miRNA结合,并产生可通过CHA反应放大的荧光信号,从而实现外泌体miRNA的原位高灵敏度检测。在最佳条件下,对三种外泌体miRNA的检测限为5 aM,比定量实时聚合酶链反应(qRT-PCR)低一个数量级。结合线性判别分析算法,可100%准确区分五种外泌体。重要的是,通过检测临床血浆中的外泌体miRNA,对64例患者的包括乳腺癌、肺癌、肝癌、宫颈癌和结肠癌在内的五种癌症进行区分,准确率达99%。这种简单、准确且灵敏的生物传感器有潜力扩展为临床非侵入性癌症诊断测试。

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