Communications Biology (Jul 2024)

Normoglycemia and physiological cortisone level maintain glucose homeostasis in a pancreas-liver microphysiological system

  • Sophie Rigal,
  • Belén Casas,
  • Kajsa P. Kanebratt,
  • Charlotte Wennberg Huldt,
  • Lisa U. Magnusson,
  • Erik Müllers,
  • Fredrik Karlsson,
  • Maryam Clausen,
  • Sara F. Hansson,
  • Louise Leonard,
  • Jonathan Cairns,
  • Rasmus Jansson Löfmark,
  • Carina Ämmälä,
  • Uwe Marx,
  • Peter Gennemark,
  • Gunnar Cedersund,
  • Tommy B. Andersson,
  • Liisa K. Vilén

DOI
https://doi.org/10.1038/s42003-024-06514-w
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 23

Abstract

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Abstract Current research on metabolic disorders and diabetes relies on animal models because multi-organ diseases cannot be well studied with standard in vitro assays. Here, we have connected cell models of key metabolic organs, the pancreas and liver, on a microfluidic chip to enable diabetes research in a human-based in vitro system. Aided by mechanistic mathematical modeling, we demonstrate that hyperglycemia and high cortisone concentration induce glucose dysregulation in the pancreas-liver microphysiological system (MPS), mimicking a diabetic phenotype seen in patients with glucocorticoid-induced diabetes. In this diseased condition, the pancreas-liver MPS displays beta-cell dysfunction, steatosis, elevated ketone-body secretion, increased glycogen storage, and upregulated gluconeogenic gene expression. Conversely, a physiological culture condition maintains glucose tolerance and beta-cell function. This method was reproducible in two laboratories and was effective in multiple pancreatic islet donors. The model also provides a platform to identify new therapeutic proteins, as demonstrated with a combined transcriptome and proteome analysis.