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Journal article

Impedimetric toxicity assay in microfluidics using free and liposome-encapsulated anticancer drugs

From

Department of Micro- and Nanotechnology, Technical University of Denmark1

Nanoprobes, Department of Micro- and Nanotechnology, Technical University of Denmark2

University of Siena3

Molecular Windows, Department of Micro- and Nanotechnology, Technical University of Denmark4

Colloids and Biological Interfaces, Department of Micro- and Nanotechnology, Technical University of Denmark5

Bioanalytics, Department of Micro- and Nanotechnology, Technical University of Denmark6

Polytechnic University of Milan7

University of Genoa8

In this work, we have developed a microfluidic cytotoxicity assay for a cell culture and detection platform, which enables both fluid handling and electrochemical/optical detection. The cytotoxic effect of anticancer drugs doxorubicin (DOX), oxaliplatin (OX) as well as OX-loaded liposomes, developed for targeted drug delivery, was evaluated using real-time impedance monitoring.

The time-dependent effect of DOX on HeLa cells was monitored and found to have a delayed onset of cytotoxicity in microfluidics compared with static culture conditions based on data obtained in our previous study. The result of a fluorescent microscopic annexin V/propidium iodide assay, performed in microfluidics, confirmed the outcome of the real-time impedance assay.

In addition, the response of HeLa cells to OX-induced cytotoxicity proved to be slower than toxicity induced by DOX. A difference in the time-dependent cytotoxic response of fibrosarcoma cells (HT1080) to free OX and OX-loaded liposomes was observed and attributed to incomplete degradation of the liposomes, which results in lower drug availability.

The matrix metalloproteinase (MMP)-dependent release of OX from OX-loaded liposomes was also confirmed using laryngopharynx carcinoma cells (FaDu). The comparison and the observed differences between the cytotoxic effects under microfluidic and static conditions highlight the importance of comparative studies as basis for implementation of microfluidic cytotoxic assays.

Language: English
Year: 2015
Pages: 2204-2212
ISSN: 15206882 , 00032700 and 15204782
Types: Journal article
DOI: 10.1021/ac503621d
ORCIDs: Zor, Kinga , Melander, Fredrik , Heiskanen, Arto , Andresen, Thomas Lars and Emnéus, Jenny

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