Abstract

In this study, we have employed several in vitro models to study the factors involved in the differentiation of pancreatic precursor cells into hormone-producing cells of the islets of Langerhans and their mechanisms of action. Development of the endocrine pancreas includes a series of early events wherein precursor cells migrate to form aggregates that subsequently differentiate into islets of Langerhans. We used PANC-1 cells, a human pancreatic cell line that can be induced to differentiate into hormone-producing cell aggregates, to study regulation of cell migration and aggregation that precedes differentiation. We showed that exogenous fibroblast growth factor-2 (FGF2) was an effective chemoattractant for PANC-1 cells. We developed the following evidence that FGF2 is a paracrine stimulator of migration and aggregation of PANC-1 cells: 1) FGF2 is produced and secreted by a subset of these cells; 2) inhibition of FGF receptor tyrosine kinase inhibits cell migration and aggregate formation; 3) a subset of cells express FGF receptors-2, -3 and -4; 4) secreted FGF2 is bound to the extracellular matrix; and 5) FGF2 neutralizing antibody inhibits cell migration, an essential step in aggregate formation. We suggest that paracrine factors, such as FGF2, are important extracellular regulators of the early steps of human pancreatic precursor cell development into hormone-expressing islets in culture. These findings may provide insights that will facilitate generation of islet cells in vitro that could be used for replacement therapy of type 1 diabetes in humans. Cell-cell and cell-matrix interactions, which may be regulated by modulating the expression or activity of cell adhesion molecules, play important roles in embryonic development. Neural cell adhesion molecule (NCAM) is involved in development of the endocrine pancreas in rodents but its role in human pancreatic development is unclear. As islets of Langerhans may originate from undifferentiated progenitor cells resident in pancreatic ducts, we recently established a protocol in which human pancreatic ductal carcinoma PANC-1 cells are induced to differentiate in vitro into hormone-producing islet-like cell aggregates (ICAs). We studied the role of NCAM in PANC-1 cells during their differentiation. Within 24 hours of induction of differentiation, expression of NCAM mRNA increased and cells exhibited increased adherence to a collagen IV matrix. NCAM was concentrated at the periphery of cells in ICAs, in a pattern similar to adult human islets, whereas it was absent or diffusely expressed in undifferentiated PANC-1 cells. NCAM is involved in cell-matrix and cell-cell interactions because anti-NCAM antibody reduced adhesion of cells from ICAs to collagen IV, fibronectin and vitronectin and caused a reduction in the mean size of ICAs from 130 ?m to 60 ?m. Our data show that NCAM is needed for aggregation of islet cell precursors and suggest that NCAM is essential for the normal architecture of mature islets in humans. These initial studies have allowed us to establish in vitro cell systems in which we can study the factors that regulate differentiation of endocrine pancreas precursor cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Intramural Research (Z01)
Project #
1Z01DK011007-01
Application #
6673630
Study Section
(RHA)
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
U.S. National Inst Diabetes/Digst/Kidney
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Hiram-Bab, Sahar; Katz, Liora S; Shapira, Hagit et al. (2014) Platelet-derived growth factor BB mimics serum-induced dispersal of pancreatic epithelial cell clusters. J Cell Physiol 229:743-51
Katz, Liora S; Geras-Raaka, Elizabeth; Gershengorn, Marvin C (2013) Reprogramming adult human dermal fibroblasts to islet-like cells by epigenetic modification coupled to transcription factor modulation. Stem Cells Dev 22:2551-60
Couty, Jean-Pierre; Lupu-Meiri, Monica; Oron, Yoram et al. (2009) Kaposi's sarcoma-associated herpesvirus-G protein-coupled receptor-expressing endothelial cells exhibit reduced migration and stimulated chemotaxis by chemokine inverse agonists. J Pharmacol Exp Ther 329:1142-7
Ikonomou, L; Geras-Raaka, E; Raaka, B M et al. (2008) Beta-catenin signalling in mesenchymal islet-derived precursor cells. Cell Prolif 41:474-91
Deshet, Naamit; Lupu-Meiri, Monica; Espinoza, Ingrid et al. (2008) Plasminogen-induced aggregation of PANC-1 cells requires conversion to plasmin and is inhibited by endogenous plasminogen activator inhibitor-1. J Cell Physiol 216:632-9
Mutskov, Vesco; Raaka, Bruce M; Felsenfeld, Gary et al. (2007) The human insulin gene displays transcriptionally active epigenetic marks in islet-derived mesenchymal precursor cells in the absence of insulin expression. Stem Cells 25:3223-33
Morton, Russell A; Geras-Raaka, Elizabeth; Wilson, Leah M et al. (2007) Endocrine precursor cells from mouse islets are not generated by epithelial-to-mesenchymal transition of mature beta cells. Mol Cell Endocrinol 270:87-93
Davani, Behrous; Ikonomou, Laertis; Raaka, Bruce M et al. (2007) Human islet-derived precursor cells are mesenchymal stromal cells that differentiate and mature to hormone-expressing cells in vivo. Stem Cells 25:3215-22
Wei, Chiju; Geras-Raaka, Elizabeth; Marcus-Samuels, Bernice et al. (2006) Trypsin and thrombin accelerate aggregation of human endocrine pancreas precursor cells. J Cell Physiol 206:322-8
Gershengorn, Marvin C; Geras-Raaka, Elizabeth; Hardikar, Anandwardhan A et al. (2005) Are better islet cell precursors generated by epithelial-to-mesenchymal transition? Cell Cycle 4:380-2

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