Issue 21, 2016
From the journal:

Analyst

Recognition of tumor cells by immuno-SERS-markers in a microfluidic chip at continuous flow

I. Freitag,a   C. Beleites,ab   S. Dochow,a   J. H. Clement,c   C. Krafft*a  and  J. Poppad  

* Corresponding authors

a Leibniz Institute of Photonic Technology, Albert-Einstein-Str. 9, D-07745 Jena, Germany
E-mail: christoph.krafft@leibniz-ipht.de

b Claudia Beleites Chemometric Consulting and Chemometrix GmbH, Södeler Weg 19, D-61200 Wölfersheim, Germany

c Department of Internal Medicine II, Haematology and Medical Oncology, University Hospital, Jena, Germany

d Institute of Physical Chemistry and Abbe Center of Photonics, FSU Jena, Helmholtzweg 4, D-07743 Jena, Germany

Abstract

SERS active nanoparticles were labeled with a reporter molecule and conjugated with anti-EpCAM antibodies. These immuno SERS markers were mixed with leukocytes, MCF-7 breast cancer cells and polystyrene beads, and the mixture was injected into a microfluidic quartz chip. Raman spectra were acquired at 785 nm excitation with 25 milliseconds exposure time in a continuous flow regime. Spectral unmixing by N-FINDR identified spectral signatures of SERS-labelled cells and polystyrene beads. This approach demonstrated rapid and reproducible SERS-assisted cell detection. Strategies are discussed to further increase the throughput for cell sorting.

Graphical abstract: Recognition of tumor cells by immuno-SERS-markers in a microfluidic chip at continuous flow

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Article information

DOI
https://doi.org/10.1039/C6AN01739H
Article type
Communication
Submitted
01 Aug 2016
Accepted
27 Sep 2016
First published
27 Sep 2016

Analyst, 2016,141, 5986-5989

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Recognition of tumor cells by immuno-SERS-markers in a microfluidic chip at continuous flow

I. Freitag, C. Beleites, S. Dochow, J. H. Clement, C. Krafft and J. Popp, Analyst, 2016, 141, 5986 DOI: 10.1039/C6AN01739H

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