JCI Insight (Mar 2021)

Adipocyte-derived extracellular vesicles regulate survival and function of pancreatic β cells

  • Iacopo Gesmundo,
  • Barbara Pardini,
  • Eleonora Gargantini,
  • Giacomo Gamba,
  • Giovanni Birolo,
  • Alessandro Fanciulli,
  • Dana Banfi,
  • Noemi Congiusta,
  • Enrica Favaro,
  • Maria Chiara Deregibus,
  • Gabriele Togliatto,
  • Gaia Zocaro,
  • Maria Felice Brizzi,
  • Raul M. Luque,
  • Justo P. Castaño,
  • Maria Alessandra Bocchiotti,
  • Simone Arolfo,
  • Stefania Bruno,
  • Rita Nano,
  • Mario Morino,
  • Lorenzo Piemonti,
  • Huy Ong,
  • Giuseppe Matullo,
  • Juan M. Falcón-Pérez,
  • Ezio Ghigo,
  • Giovanni Camussi,
  • Riccarda Granata

Journal volume & issue
Vol. 6, no. 5

Abstract

Read online

Extracellular vesicles (EVs) are implicated in the crosstalk between adipocytes and other metabolic organs, and an altered biological cargo has been observed in EVs from human obese adipose tissue (AT). Yet, the role of adipocyte-derived EVs in pancreatic β cells remains to be determined. Here, we explored the effects of EVs released from adipocytes isolated from both rodents and humans and human AT explants on survival and function of pancreatic β cells and human pancreatic islets. EVs from healthy 3T3-L1 adipocytes increased survival and proliferation and promoted insulin secretion in INS-1E β cells and human pancreatic islets, both those untreated or exposed to cytokines or glucolipotoxicity, whereas EVs from inflamed adipocytes caused β cell death and dysfunction. Human lean adipocyte-derived EVs produced similar beneficial effects, whereas EVs from obese AT explants were harmful for human EndoC-βH3 β cells. We observed differential expression of miRNAs in EVs from healthy and inflamed adipocytes, as well as alteration in signaling pathways and expression of β cell genes, adipokines, and cytokines in recipient β cells. These in vitro results suggest that, depending on the physiopathological state of AT, adipocyte-derived EVs may influence β cell fate and function.

Keywords