| Literature DB >> 24726385 |
Ulrika Krus1, Ben C King2, Vini Nagaraj1, Nikhil R Gandasi3, Jonatan Sjölander2, Pawel Buda1, Eliana Garcia-Vaz1, Maria F Gomez1, Emilia Ottosson-Laakso1, Petter Storm1, Malin Fex1, Petter Vikman1, Enming Zhang1, Sebastian Barg3, Anna M Blom4, Erik Renström5.
Abstract
Type 2 diabetes is triggered by reduced insulin production, caused by genetic and environmental factors such as inflammation originating from the innate immune system. Complement proteins are a component of innate immunity and kill non-self cells by perforating the plasma membrane, a reaction prevented by CD59. Human pancreatic islets express CD59 at very high levels. CD59 is primarily known as a plasma membrane protein in membrane rafts, but most CD59 protein in pancreatic β cells is intracellular. Removing extracellular CD59 disrupts membrane rafts and moderately stimulates insulin secretion, whereas silencing intracellular CD59 markedly suppresses regulated secretion by exocytosis, as demonstrated by TIRF imaging. CD59 interacts with the exocytotic proteins VAMP2 and Syntaxin-1. CD59 expression is reduced by glucose and in rodent diabetes models but upregulated in human diabetic islets, potentially reflecting compensatory reactions. This unconventional action of CD59 broadens the established view of innate immunity in type 2 diabetes.Entities:
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Year: 2014 PMID: 24726385 DOI: 10.1016/j.cmet.2014.03.001
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287