1. Academic Validation
  2. Sustained proliferation of PDX-1+ cells derived from human islets

Sustained proliferation of PDX-1+ cells derived from human islets

  • Diabetes. 1999 May;48(5):1013-9. doi: 10.2337/diabetes.48.5.1013.
G M Beattie 1 P Itkin-Ansari V Cirulli G Leibowitz A D Lopez S Bossie M I Mally F Levine A Hayek
Affiliations

Affiliation

  • 1 Department of Pediatrics, University of California at San Diego, USA.
Abstract

Ex vivo expansion of human beta-cells is an important step toward the development of cell-based Insulin delivery systems in type 1 diabetes. Here, we report that human pancreatic endocrine cells can be expanded through 15 cell doublings in vitro for an estimated total 30,000-fold increase in cell number. We believe that the cells resulting from these cultures are of beta-cell origin, since they uniformly express the transcription factor PDX-1 (STF-1, IDX-1, IPF-1), which is initially seen only in cells positive for Insulin and negative for the ductal cell marker cytokeratin (CK)-19. To rule out the possibility that PDX-1 expression might be induced by the culture conditions used here, cells from isolated human pancreatic ducts were cultured under the same conditions as the islet cells. Cells in these cultures expressed CK-19 but not PDX-1. Although the expanded beta-cells continued to express PDX-1, Insulin expression was lost over time. Whether reexpression of islet-specific genes in vitro is essential for successful cell transplantation remains to be determined.

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