Cell Reports (Aug 2017)

αE-Catenin Is a Positive Regulator of Pancreatic Islet Cell Lineage Differentiation

  • Antonio J. Jimenez-Caliani,
  • Rudolf Pillich,
  • Wendy Yang,
  • Giuseppe R. Diaferia,
  • Paolo Meda,
  • Laura Crisa,
  • Vincenzo Cirulli

DOI
https://doi.org/10.1016/j.celrep.2017.07.035
Journal volume & issue
Vol. 20, no. 6
pp. 1295 – 1306

Abstract

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The development and function of epithelia depend on the establishment and maintenance of cell-cell adhesion and intercellular junctions, which operate as mechanosensor hubs for the transduction of biochemical signals regulating cell proliferation, differentiation, survival, and regeneration. Here, we show that αE-catenin, a key component of adherens junctions, functions as a positive regulator of pancreatic islet cell lineage differentiation by repressing the sonic hedgehog pathway (SHH). Thus, deletion of αE-catenin in multipotent pancreatic progenitors resulted in (1) loss of adherens junctions, (2) constitutive activation of SHH, (3) decrease in islet cell lineage differentiation, and (4) accumulation of immature Sox9+ progenitors. Pharmacological blockade of SHH signaling in pancreatic organ cultures and in vivo rescued this defect, allowing αE-catenin-null Sox9+ pancreatic progenitors to differentiate into endocrine cells. The results uncover crucial functions of αE-catenin in pancreatic islet development and harbor significant implications for the design of β cell replacement and regeneration therapies in diabetes.

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