Abstract
microRNAs (miRNAs) play important roles in pancreas development and in regulation of insulin expression in the adult. Here we show that loss of miRNAs activity in beta-cells during embryonic development results in lower beta-cell mass and in impaired glucose tolerance. Dicer1-null cells initially constitute a significant portion of the total beta-cell population. However, during postnatal development, Dicer1-null cells are depleted. Furthermore, wild-type beta cells are repopulating the islets in complex compensatory dynamics. Because loss of Dicer1 is also associated with changes in the distribution of membranous E-cadherin, we hypothesized that E-cadherin activity may play a role in beta cell survival or islet architecture. However, genetic loss of E-cadherin function does not impair islet architecture, suggesting that miRNAs likely function through other or redundant effectors in the endocrine pancreas.
Publication types
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Research Support, Non-U.S. Gov't
MeSH terms
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Animals
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Apoptosis
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Blood Glucose / analysis
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Cadherins / genetics
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Cadherins / metabolism
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Crosses, Genetic
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DEAD-box RNA Helicases / genetics
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DEAD-box RNA Helicases / metabolism*
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Gene Expression Regulation, Developmental
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Glucose Intolerance / blood
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Glucose Intolerance / metabolism*
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Glucose Intolerance / pathology*
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Heterozygote
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Insulin / blood
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Insulin / metabolism
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Insulin Secretion
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Insulin-Secreting Cells / metabolism*
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Insulin-Secreting Cells / pathology*
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Integrases / genetics
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Integrases / metabolism
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Islets of Langerhans / growth & development
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Islets of Langerhans / metabolism
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Islets of Langerhans / pathology
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Male
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Mice
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Mice, Knockout
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Mice, Transgenic
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MicroRNAs / metabolism*
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Mutation
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Organogenesis
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Ribonuclease III / genetics
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Ribonuclease III / metabolism*
Substances
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Blood Glucose
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Cadherins
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Insulin
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MicroRNAs
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Cre recombinase
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Integrases
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Dicer1 protein, mouse
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Ribonuclease III
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DEAD-box RNA Helicases