β-arrestin-2 is an essential regulator of pancreatic β-cell function under physiological and pathophysiological conditions.
Lu ZhuJoana AlmaçaPrasanna K DadiHao HongWataru SakamotoMario RossiRegina J LeeNicholas C VierraHuiyan LuYinghong CuiSara M McMillinNicole A PerryVsevolod V GurevichAmy LeeBryan KuoRichard D LeapmanFranz M MatschinskyNicolai M DolibaNikhil M UrsMarc G CaronDavid A JacobsonAlejandro CaicedoJürgen WessPublished in: Nature communications (2017)
β-arrestins are critical signalling molecules that regulate many fundamental physiological functions including the maintenance of euglycemia and peripheral insulin sensitivity. Here we show that inactivation of the β-arrestin-2 gene, barr2, in β-cells of adult mice greatly impairs insulin release and glucose tolerance in mice fed with a calorie-rich diet. Both glucose and KCl-induced insulin secretion and calcium responses were profoundly reduced in β-arrestin-2 (barr2) deficient β-cells. In human β-cells, barr2 knockdown abolished glucose-induced insulin secretion. We also show that the presence of barr2 is essential for proper CAMKII function in β-cells. Importantly, overexpression of barr2 in β-cells greatly ameliorates the metabolic deficits displayed by mice consuming a high-fat diet. Thus, our data identify barr2 as an important regulator of β-cell function, which may serve as a new target to improve β-cell function.
Keyphrases
- induced apoptosis
- high fat diet
- cell cycle arrest
- type diabetes
- transcription factor
- endoplasmic reticulum stress
- adipose tissue
- oxidative stress
- traumatic brain injury
- physical activity
- weight loss
- skeletal muscle
- diabetic rats
- dna methylation
- high glucose
- metabolic syndrome
- electronic health record
- endothelial cells
- genome wide