Rapid Biofabrication of an Advanced Microphysiological System Mimicking Phenotypical Heterogeneity and Drug Resistance in Glioblastoma

Author:

Pun Sirjana1ORCID,Prakash Anusha12,Demaree Dalee13,Krummel Daniel Pomeranz45ORCID,Sciumè Giuseppe6,Sengupta Soma4578,Barrile Riccardo19ORCID

Affiliation:

1. Department of Biomedical Engineering University of Cincinnati Cincinnati OH 45221 USA

2. Abbvie Worcester Massachusetts 01605 USA

3. Thermo Fisher Scientific Waltham Massachusetts 02451 USA

4. Department of Neurology University of Cincinnati Cincinnati OH 45219 USA

5. Department of Neurosurgery University of North Carolina Chapel Hill NC 27599 USA

6. Institute of Mechanics and Engineering‐12 M University of Bordeaux Bordeaux 33607 France

7. Department of Neurology University of North Carolina Chapel Hill NC 27599‐7025 USA

8. Lineberger Comprehensive Cancer Center University of North Carolina Chapel Hill NC 27599‐7295 USA

9. Center for Stem Cells and Organoid Medicine (CuSTOM) Cincinnati Children's Hospital Medical Center Cincinnati OH 45229 USA

Abstract

AbstractMicrophysiological systems (MPSs) reconstitute tissue interfaces and organ functions, presenting a promising alternative to animal models in drug development. However, traditional materials like polydimethylsiloxane (PDMS) often interfere by absorbing hydrophobic molecules, affecting drug testing accuracy. Additive manufacturing, including 3D bioprinting, offers viable solutions. GlioFlow3D, a novel microfluidic platform combining extrusion bioprinting and stereolithography (SLA) is introduced. GlioFlow3D integrates primary human cells and glioblastoma (GBM) lines in hydrogel‐based microchannels mimicking vasculature, within an SLA resin framework using cost‐effective materials. The study introduces a robust protocol to mitigate SLA resin cytotoxicity. Compared to PDMS, GlioFlow3D demonstrated lower small molecule absorption, which is relevant for accurate testing of small molecules like Temozolomide (TMZ). Computational modeling is used to optimize a pumpless setup simulating interstitial fluid flow dynamics in tissues. Co‐culturing GBM with brain endothelial cells in GlioFlow3D showed enhanced CD133 expression and TMZ resistance near vascular interfaces, highlighting spatial drug resistance mechanisms. This PDMS‐free platform promises advanced drug testing, improving preclinical research and personalized therapy by elucidating complex GBM drug resistance mechanisms influenced by the tissue microenvironment.

Publisher

Wiley

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