miR-17-92 and miR-106b-25 clusters regulate beta cell mitotic checkpoint and insulin secretion in mice

Diabetologia. 2019 Sep;62(9):1653-1666. doi: 10.1007/s00125-019-4916-z. Epub 2019 Jun 11.

Abstract

Aims/hypothesis: Adult beta cells in the pancreas are the sole source of insulin in the body. Beta cell loss or increased demand for insulin impose metabolic challenges because adult beta cells are generally quiescent and infrequently re-enter the cell division cycle. The aim of this study is to test the hypothesis that a family of proto-oncogene microRNAs that includes miR-17-92 and miR-106b-25 clusters regulates beta cell proliferation or function in the adult endocrine pancreas.

Methods: To elucidate the role of miR-17-92 and miR-106b-25 clusters in beta cells, we used a conditional miR-17-92/miR-106b-25 knockout mouse model. We employed metabolic assays in vivo and ex vivo, together with advanced microscopy of pancreatic sections, bioinformatics, mass spectrometry and next generation sequencing, to examine potential targets of miR-17-92/miR-106b-25, by which they might regulate beta cell proliferation and function.

Results: We demonstrate that miR-17-92/miR-106b-25 regulate the adult beta cell mitotic checkpoint and that miR-17-92/miR-106b-25 deficiency results in reduction in beta cell mass in vivo. Furthermore, we reveal a critical role for miR-17-92/miR-106b-25 in glucose homeostasis and in controlling insulin secretion. We identify protein kinase A as a new relevant molecular pathway downstream of miR-17-92/miR-106b-25 in control of adult beta cell division and glucose homeostasis.

Conclusions/interpretation: The study contributes to the understanding of proto-oncogene miRNAs in the normal, untransformed endocrine pancreas and illustrates new genetic means for regulation of beta cell mitosis and function by non-coding RNAs.

Data availability: Sequencing data that support the findings of this study have been deposited in GEO with the accession code GSE126516.

Keywords: Beta cells; Cell cycle; Diabetes; GSIS; Glucose-stimulated insulin secretion; PKA; Protein kinase A; microRNA.

Publication types

  • Research Support, Non-U.S. Gov't

MeSH terms

  • Animals
  • Cells, Cultured
  • Female
  • Flow Cytometry
  • Insulin Secretion / genetics
  • Insulin Secretion / physiology*
  • Insulin-Secreting Cells / metabolism*
  • Male
  • Mass Spectrometry
  • Mice
  • MicroRNAs / genetics
  • MicroRNAs / metabolism*
  • Mitosis / genetics
  • Mitosis / physiology
  • Pancreas / metabolism

Substances

  • MIRN17-92 microRNA, mouse
  • MicroRNAs
  • Mirn106 microRNA, mouse