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Enabling cell recovery from 3D cell culture microfluidic devices for tumour microenvironment biomarker profiling.


ABSTRACT: The tumour microenvironment (TME) has recently drawn much attention due to its profound impact on tumour development, drug resistance and patient outcome. There is an increasing interest in new therapies that target the TME. Nonetheless, most established in vitro models fail to include essential cues of the TME. Microfluidics can be used to reproduce the TME in vitro and hence provide valuable insight on tumour evolution and drug sensitivity. However, microfluidics remains far from well-established mainstream molecular and cell biology methods. Therefore, we have developed a quick and straightforward collagenase-based enzymatic method to recover cells embedded in a 3D hydrogel in a microfluidic device with no impact on cell viability. We demonstrate the validity of this method on two different cell lines in a TME microfluidic model. Cells were successfully retrieved with high viability, and we characterised the different cell death mechanisms via AMNIS image cytometry in our model.

SUBMITTER: Virumbrales-Munoz M 

PROVIDER: S-EPMC6470149 | biostudies-literature | 2019 Apr

REPOSITORIES: biostudies-literature

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Enabling cell recovery from 3D cell culture microfluidic devices for tumour microenvironment biomarker profiling.

Virumbrales-Muñoz María M   Ayuso Jose M JM   Lacueva Alodia A   Randelovic Teodora T   Livingston Megan K MK   Beebe David J DJ   Oliván Sara S   Pereboom Desirée D   Doblare Manuel M   Fernández Luis L   Ochoa Ignacio I  

Scientific reports 20190417 1


The tumour microenvironment (TME) has recently drawn much attention due to its profound impact on tumour development, drug resistance and patient outcome. There is an increasing interest in new therapies that target the TME. Nonetheless, most established in vitro models fail to include essential cues of the TME. Microfluidics can be used to reproduce the TME in vitro and hence provide valuable insight on tumour evolution and drug sensitivity. However, microfluidics remains far from well-establis  ...[more]

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