Regulation of PKD by the MAPK p38δ in Insulin Secretion and Glucose Homeostasis
Abstract
Dysfunction and loss of insulin-producing pancreatic β cells represent hallmarks of diabetes mellitus. Here, we show that mice lacking the mitogen-activated protein kinase (MAPK) p38δ display improved glucose tolerance due to enhanced insulin secretion from pancreatic β cells. Deletion of p38δ results in pronounced activation of protein kinase D (PKD), the latter of which we have identified as a pivotal regulator of stimulated insulin exocytosis. p38δ catalyzes an inhibitory phosphorylation of PKD1, thereby attenuating stimulated insulin secretion. In addition, p38δ null mice are protected against high-fat-feeding-induced insulin resistance and oxidative stress-mediated β cell failure. Inhibition of PKD1 reverses enhanced insulin secretion from p38δ-deficient islets and glucose tolerance in p38δ null mice as well as their susceptibility to oxidative stress. In conclusion, the p38δ-PKD pathway integrates regulation of the insulin secretory capacity and survival of pancreatic β cells, pointing to a pivotal role for this pathway in the development of overt diabetes mellitus. Show more
Permanent link
https://doi.org/10.3929/ethz-b-000513554Publication status
publishedJournal / series
CellVolume
Pages / Article No.
Publisher
Cell PressSubject
Signlaing; Cellbio; HumdiseaseOrganisational unit
03770 - Ricci, Romeo (SNF-Professur)
03663 - Aebersold, Rudolf (emeritus) / Aebersold, Rudolf (emeritus)
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