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A microfluidic impedance-based extended infectivity assay: combining retroviral amplification and cytopathic effect monitoring on a single lab-on-a-chip platform

  • Detection, quantification and monitoring of virus – host cell interactions are of great importance when evaluating the safety of pharmaceutical products. With the wide usage of viral based vector systems in combination with mammalian cell lines for the production of biopharmaceuticals, the presence of replication competent viral particles needs to be avoided and potential hazards carefully assessed. Consequently, regulatory agencies recommend viral clearance studies using plaque assays or TCID50 assays to evaluate the efficiency of the production process in removing viruses. While plaque assays provide reliable information on the presence of viral contaminations, they are still tedious to perform and can take up to two weeks to finish. To overcome some of these limitations, we have automated, miniaturized and integrated the dual cell culture bioassay into a common lab-on-a-chip platform containing embedded electrical sensor arrays to enrich and detect infectious viruses. Results of our microfluidic single step assay show that a significant reduction in assay time down to 3 to 4 days can be achieved using simultaneous cell-based viral amplification, release and detection of cytopathic effects in a target cell line. We further demonstrate the enhancing effect of continuous fluid flow on infection of PG-4 reporter cells by newly formed and highly active virions by M. dunni cells, thus pointing to the importance of physical relevant viral–cell interactions.

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Metadaten
Author:Michaela Purtscher, Mario Rothbauer, Sebastian Rudi Adam Kratz, Andrew Bailey, Peter Lieberzeit, Peter Ertl
Parent Title (English):Lab on a Chip
Document Type:Article
Language:English
Completed Date:2021/02/01
Date of first Publication:2021/07/13
Responsibility for metadata:Fachhochschule Technikum Wien
Release Date:2021/07/13
GND Keyword:Lab on Chip; Microfluidics; Tissue Engineering
Volume:2021
Issue:Issue 7
First Page:1364
Last Page:1372
Publish on Website:1
Open Access:1
Reviewed:1
Link to Publication:https://pubs.rsc.org/en/content/articlelanding/2021/LC/D0LC01056A#!divAbstract
Link to Publication:https://zenodo.org/record/5081887#.YOa5LjNxc2w
Department:Department Life Science Engineering
Research Focus:Tissue Engineering & Molecular Life Science Technologies
Projects:Eigenmittel
Studienjahr:2021/2022