Literature DB >> 23354125

Molecular basis for the regulation of islet beta cell mass in mice: the role of E-cadherin.

N Wakae-Takada1, S Xuan, K Watanabe, P Meda, R L Leibel.   

Abstract

AIMS/HYPOTHESIS: In rodents and humans, the rate of beta cell proliferation declines rapidly after birth; formation of the islets of Langerhans begins perinatally and continues after birth. Here, we tested the hypothesis that increasing levels of E-cadherin during islet formation mediate the decline in beta cell proliferation rate by contributing to a reduction of nuclear β-catenin and D-cyclins.
METHODS: We examined E-cadherin, nuclear β-catenin, and D-cyclin levels, as well as cell proliferation during in vitro and in vivo formation of islet cell aggregates, using β-TC6 cells and transgenic mice with green fluorescent protein (GFP)-labelled beta cells, respectively. We tested the role of E-cadherin using antisense-mediated reductions of E-cadherin in β-TC6 cells, and mice segregating for a beta cell-specific E-cadherin knockout (Ecad [also known as Cdh1] βKO).
RESULTS: In vitro, pseudo-islets of β-TC6 cells displayed increased E-cadherin but decreased nuclear β-catenin and cyclin D2, and reduced rates of cell proliferation, compared with monolayers. Antisense knockdown of E-cadherin increased cell proliferation and levels of cyclins D1 and D2. After birth, beta cells showed increased levels of E-cadherin, but decreased levels of D-cyclin, whereas islets of Ecad βKO mice showed increased levels of D-cyclins and nuclear β-catenin, as well as increased beta cell proliferation. These islets were significantly larger than those of control mice and displayed reduced levels of connexin 36. These changes correlated with reduced insulin response to ambient glucose, both in vitro and in vivo. CONCLUSIONS/
INTERPRETATION: The findings support our hypothesis by indicating an important role of E-cadherin in the control of beta cell mass and function.

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Year:  2013        PMID: 23354125      PMCID: PMC3927460          DOI: 10.1007/s00125-012-2824-6

Source DB:  PubMed          Journal:  Diabetologia        ISSN: 0012-186X            Impact factor:   10.122


  45 in total

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3.  Cadherin engagement protects human β-cells from apoptosis.

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Review 1.  Impact of islet architecture on β-cell heterogeneity, plasticity and function.

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2.  Sustained Administration of β-cell Mitogens to Intact Mouse Islets Ex Vivo Using Biodegradable Poly(lactic-co-glycolic acid) Microspheres.

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Review 6.  Signals in the pancreatic islet microenvironment influence β-cell proliferation.

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Review 8.  Pancreatic β-cell heterogeneity in health and diabetes: classes, sources, and subtypes.

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9.  Intercellular Communication in the Islet of Langerhans in Health and Disease.

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10.  Transgene-associated human growth hormone expression in pancreatic β-cells impairs identification of sex-based gene expression differences.

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