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Integrated FET sensing microsystem for specific detection of pancreatic cancer exosomal miRNA10b

化学 微系统 外体 微泡 生物传感器 癌症生物标志物 检出限 生物标志物 纳米技术 小RNA 癌症 色谱法 生物化学 材料科学 医学 内科学 基因
作者
Yi Yu,Chunzi Liang,Qiang-Qiang Wan,Dan Jin,Xi Liu,Zhiyong Zhang,Z. J. Sun,Guo‐Jun Zhang
出处
期刊:Analytica Chimica Acta [Elsevier BV]
卷期号:1284: 341995-341995 被引量:10
标识
DOI:10.1016/j.aca.2023.341995
摘要

Tumor-derived exosome (TD-Ex) serves as a crucial early diagnostic biomarker of pancreatic cancer (PC). However, accurate identification of TD-Ex from PC is still a challenging work. In this paper, a detection microsystem that integrates magnetic separation and FET biosensor is developed, which is capable of selectively separating TD-Ex of PC from the plasma and detecting exosomal miRNA10b in a sensitive and specific manner. The magnetic beads were functionalized with dual antibody (GPC-1 antibody and EpCAM antibody), enabling selective recognition and capture of PC-derived exosomes. On the other hand, a peptide nucleic acid (PNA)- functionalized reduced graphene oxide field-effect transistor (RGO FET) biosensor was subsequently utilized to detect the exosomal miRNA10b, which is highly expressed in PC- derived exosomes. This system could achieve a low detection limit down to 78 fM, and selectively identify miRNA10b from single-base mismatched miRNA. In addition, 40 clinical plasma samples were tested with this microsystem, and the results indicate that it could effectively distinguish PC patients from healthy individuals. The assay combines specific capture and enrichment of PC-derived exosomes with sensitive and selective detection of exosomal miRNA, showing its potential to be used as an effective scheme for PC early diagnosis.
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