A Fluid Multivalent Magnetic Interface for High‐Performance Isolation and Proteomic Profiling of Tumor‐Derived Extracellular Vesicles

Isolation and analysis of tumor‐derived extracellular vesicles (T‐EVs) are important for clinical cancer management. Here, we develop a fluid multivalent magnetic interface (FluidmagFace) in a microfluidic chip for high‐performance isolation, release, and protein profiling of T‐EVs. The FluidmagFace...

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Veröffentlicht in:Angewandte Chemie 2023-05, Vol.135 (21), p.n/a
Hauptverfasser: Niu, Qi, Shu, Yun, Chen, Yuanqiang, Huang, Zhi, Yao, Zhixian, Chen, Xiaofeng, Lin, Fanghe, Feng, Jianzhou, Huang, Chen, Wang, Hua, Ding, Hongming, Yang, Chaoyong, Wu, Lingling
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container_issue 21
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container_title Angewandte Chemie
container_volume 135
creator Niu, Qi
Shu, Yun
Chen, Yuanqiang
Huang, Zhi
Yao, Zhixian
Chen, Xiaofeng
Lin, Fanghe
Feng, Jianzhou
Huang, Chen
Wang, Hua
Ding, Hongming
Yang, Chaoyong
Wu, Lingling
description Isolation and analysis of tumor‐derived extracellular vesicles (T‐EVs) are important for clinical cancer management. Here, we develop a fluid multivalent magnetic interface (FluidmagFace) in a microfluidic chip for high‐performance isolation, release, and protein profiling of T‐EVs. The FluidmagFace increases affinity by 105‐fold with fluidity‐enhanced multivalent binding to improve isolation efficiency by 13.9 % compared with a non‐fluid interface. Its anti‐adsorption property and microfluidic hydrodynamic shear minimize contamination, increasing detection sensitivity by two orders of magnitude. Moreover, its reversibility and expandability allow high‐throughput recovery of T‐EVs for mass spectrometric protein analysis. With the chip, T‐EVs were detected in all tested cancer samples with identification of differentially expressed proteins compared with healthy controls. The FluidmagFace opens a new avenue to isolation and release of targets for cancer diagnosis and biomarker discovery. A fluid multivalent magnetic interface was engineered in a microfluidic chip to improve the kinetics and thermodynamics of biomolecular recognition for efficient isolation of tumor‐derived extracellular vesicles (T‐EVs). With the assistance of magnetic and flow fields, this interface balanced affinity, selectivity, reversibility, and extendibility, enabling high‐throughput recovery of T‐EVs for protein profiling.
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subjects Biomarkers
Cancer
Chemistry
Contamination
Extracellular Vesicles
Fluid Interface
Fluidity
Interfacial Reaction
Liquid Biopsy
Microfluidics
Protein folding
Proteins
Proteomics
Spectrometry
Tumors
Vesicles
title A Fluid Multivalent Magnetic Interface for High‐Performance Isolation and Proteomic Profiling of Tumor‐Derived Extracellular Vesicles
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