Literature DB >> 23628845

Simultaneous capture and in situ analysis of circulating tumor cells using multiple hybrid nanoparticles.

Hun Joo Lee1, Hyeon-Yeol Cho, Jin Ho Oh, Kak Namkoong, Jeong Gun Lee, Jong-Myeon Park, Soo Suk Lee, Nam Huh, Jeong-Woo Choi.   

Abstract

Using hybrid nanoparticles (HNPs), we demonstrate simultaneous capture, in situ protein expression analysis, and cellular phenotype identification of circulating tumor cells (CTCs). Each HNP consists of three parts: (i) antibodies that bind specifically to a known biomarker for CTCs, (ii) a quantum dot that emits fluorescence signals, and (iii) biotinylated DNA that allows capture and release of CTC-HNP complex to an in-house developed capture & recovery chip (CRC). To evaluate our approach, cells representative of different breast cancer subtypes (MCF-7: luminal; SK-BR-3: HER2; and MDA-MB-231: basal-like) were captured onto CRC and expressions of EpCAM, HER2, and EGFR were detected concurrently. The average capture efficiency of CTCs was 87.5% with identification accuracy of 92.4%. Subsequently, by cleaving the DNA portion with restriction enzymes, captured cells were released at efficiencies of 86.1%. Further studies showed that these recovered cells are viable and can proliferate in vitro. Using HNPs, it is possible to count, analyze in situ protein expression, and culture CTCs, all from the same set of cells, enabling a wide range of molecular- and cellular-based studies using CTCs.
Copyright © 2013 Elsevier B.V. All rights reserved.

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Year:  2013        PMID: 23628845     DOI: 10.1016/j.bios.2013.03.040

Source DB:  PubMed          Journal:  Biosens Bioelectron        ISSN: 0956-5663            Impact factor:   10.618


  14 in total

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