4.8 Article

Organoid microphysiological system preserves pancreatic islet function within 3D matrix

Journal

SCIENCE ADVANCES
Volume 7, Issue 7, Pages -

Publisher

AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/sciadv.aba5515

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Funding

  1. NIDDK supported Human Islet Research Network (HIRN) [UC4 DK104208, UG3 DK122638, F31DK118860]
  2. NIDDK-funded IIDP at City of Hope [2UC4DK098085]

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This study highlights the importance of a dynamic in vitro microenvironment for preserving the function of primary organoid models and demonstrates the utility of the MPS for in situ multiparametric assessment.
Three-dimensional (3D) multicellular organoids recapitulate the native complexities of human tissue better than traditional cellular monolayers. As organoids are insufficiently supported using standard static culture, microphysiological systems (MPSs) provide a key enabling technology to maintain organoid physiology in vitro. Here, a polydimethylsiloxane-free MPS that enables continuous dynamic culture and serial in situ multiparametric assessments was leveraged to culture organoids, specifically human and rodent pancreatic islets, within a 3D alginate hydrogel. Computational modeling predicted reduced hypoxic stress and improved insulin secretion compared to static culture. Experimental validation via serial, high-content, and noninvasive assessments quantitatively confirmed that the MPS platform retained organoid viability and functionality for at least 10 days, in stark contrast to the acute decline observed overnight under static conditions. Our findings demonstrate the importance of a dynamic in vitro microenvironment for the preservation of primary organoid function and the utility of this MPS for in situ multiparametric assessment.

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