6 research outputs found
Loss of Free Fatty Acid Receptor 2 leads to impaired islet mass and beta cell survival
Get PDFThe regulation of pancreatic β cell mass is a critical factor to help maintain normoglycemia during insulin resistance. Nutrient-sensing G protein-coupled receptors (GPCR) contribute to aspects of β cell function, including regulation of β cell mass. Nutrients such as free fatty acids (FFAs) contribute to precise regulation of β cell mass by signaling through cognate GPCRs, and considerable evidence suggests that circulating FFAs promote β cell expansion by direct and indirect mechanisms. Free Fatty Acid Receptor 2 (FFA2) is a β cell-expressed GPCR that is activated by short chain fatty acids, particularly acetate. Recent studies of FFA2 suggest that it may act as a regulator of β cell function. Here, we set out to explore what role FFA2 may play in regulation of β cell mass. Interestingly, Ffar2(-/-) mice exhibit diminished β cell mass at birth and throughout adulthood, and increased β cell death at adolescent time points, suggesting a role for FFA2 in establishment and maintenance of β cell mass. Additionally, activation of FFA2 with Gαq/11-biased agonists substantially increased β cell proliferation in in vitro and ex vivo proliferation assays. Collectively, these data suggest that FFA2 may be a novel therapeutic target to stimulate β cell growth and proliferation
An assay for small scale screening of candidate β cell proliferative factors using intact islets
No full textPropagation of the Allosteric Signal in Phosphofructokinase from Bacillus stearothermophilus
No full textIncreases in bioactive lipids accompany early metabolic changes associated with β-cell expansion in response to short-term high-fat diet
No full textHigh-fat diet-induced β-cell proliferation occurs prior to insulin resistance in C57Bl/6J male mice
No full textStructure of the apo form of Bacillus Stearothermophilus Phosphofructokinase
No full textThe crystal structure of the unliganded form of Bacillus stearothermophilus phosphofructokinase (BsPFK) was determined using molecular replacement to 2.8 Ã… resolution (Protein Data Bank entry 3U39 ). The apo BsPFK structure serves as the basis for the interpretation of any structural changes seen in the binary or ternary complexes. When the apo BsPFK structure is compared with the previously published liganded structures of BsPFK, the structural impact that the binding of the ligands produces is revealed. This comparison shows that the apo form of BsPFK resembles the substrate-bound form of BsPFK, a finding that differs from previous predictions.Rockann Mosser, Manchi C. M. Reddy, John B. Bruning, James C. Sacchettini, and Gregory D. Reinhar
