AI Article Synopsis

  • Organoids can improve the development of pancreatic progenitor cells into insulin-producing β cells, providing a platform for diabetes research.
  • The study involved creating three-dimensional pancreatic organoids using a mix of human embryonic stem cells and other cell types, then implanting them in mice for 90 days.
  • The results showed enhanced blood vessel formation and more insulin-positive cells in the organoids compared to traditional early pancreatic progenitor transplants, highlighting their potential in diabetes treatment and regenerative medicine.

Article Abstract

Organoids can be regarded as a beneficial tool for discovery of new therapeutics for diabetes and/or maturation of pancreatic progenitors (PP) towards β cells. Here, we devised a strategy to enhance maturation of PP by assembly of three-dimensional (3D) pancreatic organoids (PO) containing human embryonic stem (ES) cell derivatives including ES-derived pancreatic duodenal homeobox 1 (PDX1) early PP, mesenchymal stem cells, and endothelial cells at an optimized cell ratio, on Matrigel. The PO was placed in a 3D-printed tissue trapper and heterotopically implanted into the peritoneal cavity of immunodeficient mice where it remained for 90 days. Our results indicated that, in contrast to corresponding early PP transplants, 3D PO developed more vascularization as indicated by greater area and number of vessels, a higher number of insulin-positive cells and improvement of human C-peptide secretions. Based on our findings, PO-derived β cells could be considered a novel strategy to study human β-cell development, novel therapeutics, and regenerative medicine for diabetes.

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Source
http://dx.doi.org/10.1002/jcp.27644DOI Listing

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