Rapid Prototyping of Multilayer Microphysiological
Systems
Posted on 2020-06-03 - 15:35
Microfluidic organs-on-chips
aim to realize more biorelevant in
vitro experiments compared to traditional two-dimensional (2D) static
cell culture. Often such devices are fabricated via poly(dimethylsiloxane)
(PDMS) soft lithography, which offers benefits (e.g., high feature
resolution) along with drawbacks (e.g., prototyping time/costs). Here,
we report benchtop fabrication of multilayer, PDMS-free, thermoplastic
organs-on-chips via laser cut and assembly with double-sided adhesives
that overcome some limitations of traditional PDMS lithography. Cut
and assembled chips are economical to prototype ($2 per chip), can
be fabricated in parallel within hours, and are Luer compatible. Biocompatibility
was demonstrated with epithelial line Caco-2 cells and primary human
small intestinal organoids. Comparable to control static Transwell
cultures, Caco-2 and organoids cultured on chips formed confluent
monolayers expressing tight junctions with low permeability. Caco-2
cells-on-chip differentiated ∼4 times faster, including increased
mucus, compared to controls. To demonstrate the robustness of cut
and assemble, we fabricated a dual membrane, trilayer chip integrating
2D and 3D compartments with accessible apical and basolateral flow
chambers. As proof of concept, we cocultured a human, differentiated
monolayer and intact 3D organoids within multilayered contacting compartments.
The epithelium exhibited 3D tissue structure and organoids expanded
close to the adjacent monolayer, retaining proliferative stem cells
over 10 days. Taken together, cut and assemble offers the capability
to rapidly and economically manufacture microfluidic devices, thereby
presenting a compelling fabrication technique for developing organs-on-chips
of various geometries to study multicellular tissues.
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Hosic, Sanjin; Bindas, Adam J.; Puzan, Marissa L.; Lake, Will; Soucy, Jonathan R.; Zhou, Fanny; et al. (2020). Rapid Prototyping of Multilayer Microphysiological
Systems. ACS Publications. Collection. https://doi.org/10.1021/acsbiomaterials.0c00190