3,065 research outputs found
Weighting Background-Subtracted Events
Often a full maximum likelihood (ML) estimate is inconvenient for computational reasons (e.g., iteration over large data sets). If a variable x is a discriminating variable (s(x) 6= b(x)), a weight function can be found which allows estimation of the number of signal events with a variance approaching that of a ML estimate of the same quantity. We derive a formula and discuss it in the context of more general results on event weighting from earlier papers by Barlow and Tkachov, which also nd weighting out-performs cutting
A Proposal to Localize Fermi GBM GRBs Through Coordinated Scanning of the GBM Error Circle via Optical Telescopes
We investigate the feasibility of implementing a system that will coordinate
ground-based optical telescopes to cover the Fermi GBM Error Circle (EC). The
aim of the system is to localize GBM detected GRBs and facilitate
multi-wavelength follow-up from space and ground. This system will optimize the
observing locations in the GBM EC based on individual telescope location, Field
of View (FoV) and sensitivity. The proposed system will coordinate GBM EC
scanning by professional as well as amateur astronomers around the world. The
results of a Monte Carlo simulation to investigate the feasibility of the
project are presented.Comment: 2011 Fermi Symposium proceedings - eConf C11050
Intra-islet GLP-1, but not CCK, is necessary for β-cell function in mouse and human islets
Glucagon-like peptide 1 (GLP-1) and cholecystokinin (CCK) are gut-derived peptide hormones known to play important roles in the regulation of gastrointestinal motility and secretion, appetite, and food intake. We have previously demonstrated that both GLP-1 and CCK are produced in the endocrine pancreas of obese mice. Interestingly, while GLP-1 is well known to stimulate insulin secretion by the pancreatic β-cells, direct evidence of CCK promoting insulin release in human islets remains to be determined. Here, we tested whether islet-derived GLP-1 or CCK is necessary for the full stimulation of insulin secretion. We confirm that mouse pancreatic islets secrete GLP-1 and CCK, but only GLP-1 acts locally within the islet to promote insulin release ex vivo. GLP-1 is exclusively produced in approximately 50% of α-cells in lean mouse islets and 70% of α-cells in human islets, suggesting a paracrine α to β-cell signaling through the β-cell GLP-1 receptor. Additionally, we provide evidence that islet CCK expression is regulated by glucose, but its receptor signaling is not required during glucose-stimulated insulin secretion (GSIS). We also see no increase in GSIS in response to CCK peptides. Importantly, all these findings were confirmed in islets from non-diabetic human donors. In summary, our data suggest no direct role for CCK in stimulating insulin secretion and highlight the critical role of intra-islet GLP-1 signaling in the regulation of human β-cell function
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