Argonaute2 Mediates Compensatory Expansion of the Pancreatic b Cell

نویسندگان

  • Sudhir G. Tattikota
  • Thomas Rathjen
  • Sarah J. McAnulty
  • Hans-Hermann Wessels
  • Ildem Akerman
  • Martijn van de Bunt
  • Jean Hausser
  • Jonathan L.S. Esguerra
  • Anne Musahl
  • Amit K. Pandey
  • Xintian You
  • Wei Chen
  • Pedro L. Herrera
  • Paul R. Johnson
  • Donal O’Carroll
  • Lena Eliasson
  • Mihaela Zavolan
  • Anna L. Gloyn
  • Jorge Ferrer
  • Ruby Shalom-Feuerstein
  • Daniel Aberdam
  • Matthew N. Poy
چکیده

Pancreatic β cells adapt to compensate for increased metabolic demand during insulin resistance. Although the microRNA pathway has an essential role in β cell proliferation, the extent of its contribution is unclear. Here, we report that miR-184 is silenced in the pancreatic islets of insulin-resistant mouse models and type 2 diabetic human subjects. Reduction of miR-184 promotes the expression of its target Argonaute2 (Ago2), a component of the microRNA-induced silencing complex. Moreover, restoration of miR-184 in leptin-deficient ob/ob mice decreased Ago2 and prevented compensatory β cell expansion. Loss of Ago2 during insulin resistance blocked β cell growth and relieved the regulation of miR-375-targeted genes, including the growth suppressor Cadm1. Lastly, administration of a ketogenic diet to ob/ob mice rescued insulin sensitivity and miR-184 expression and restored Ago2 and β cell mass. This study identifies the targeting of Ago2 by miR-184 as an essential component of the compensatory response to regulate proliferation according to insulin sensitivity. TATTIKOTA, Sudhir G, et al. Argonaute2 mediates compensatory expansion of the pancreatic β cell. Cell Metabolism, 2014, vol. 19, no. 1, p. 122-34 DOI : 10.1016/j.cmet.2013.11.015

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Argonaute2 Mediates Compensatory Expansion of the Pancreatic β Cell

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تاریخ انتشار 2017