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Dive into the research topics where David Andrew Coates is active.

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Featured researches published by David Andrew Coates.


Endocrinology | 2017

Regulation of Endogenous (Male) Rodent GLP-1 Secretion and Human Islet Insulin Secretion by Antagonism of Somatostatin Receptor 5

Thomas B. Farb; Marta Adeva; Thomas James Beauchamp; Over Cabrera; David Andrew Coates; Tamika DeShea Meredith; Brian A Droz; Alexander M. Efanov; James Ficorilli; Susan L. Gackenheimer; Maria Angeles Martinez-Grau; Victoriano Molero; Gema Ruano; Michael A. Statnick; Todd M. Suter; Samreen K. Syed; Miguel A. Toledo; Francis S. Willard; Xin Zhou; Krister Bokvist; David Barrett

Incretin and insulin responses to nutrient loads are suppressed in persons with diabetes, resulting in decreased glycemic control. Agents including sulfonylureas and dipeptidyl peptidase-4 inhibitors (DPP4i) partially reverse these effects and provide therapeutic benefit; however, their modes of action limit efficacy. Because somatostatin (SST) has been shown to suppress insulin and glucagonlike peptide-1 (GLP-1) secretion through the Gi-coupled SST receptor 5 (SSTR5) isoform in vitro, antagonism of SSTR5 may improve glycemic control via intervention in both pathways. Here, we show that a potent and selective SSTR5 antagonist reverses the blunting effects of SST on insulin secretion from isolated human islets, and demonstrate that SSTR5 antagonism affords increased levels of systemic GLP-1 in vivo. Knocking out Sstr5 in mice provided a similar increase in systemic GLP-1 levels, which were not increased further by treatment with the antagonist. Treatment of mice with the SSTR5 antagonist in combination with a DPP4i resulted in increases in systemic GLP-1 levels that were more than additive and resulted in greater glycemic control compared with either agent alone. In isolated human islets, the SSTR5 antagonist completely reversed the inhibitory effect of exogenous SST-14 on insulin secretion. Taken together, these data suggest that SSTR5 antagonism should increase circulating GLP-1 levels and stimulate insulin secretion (directly and via GLP-1) in humans, improving glycemic control in patients with diabetes.


Archive | 2010

MINERALOCORTICOID RECEPTOR ANTAGONIST AND METHODS OF USE

David Andrew Coates; Konstantinos Gavardinas; Prabhakar Kondaji Jadhav


Archive | 2017

A TETRAHYDROPYRROLO[3,4-D][1,3]THIAZINE-DERIVATIVE AS BACE INHIBITOR

David Andrew Coates; Pablo Garcia Losada


Archive | 2014

3,4-DIHYDROISOQUINOLIN-2(1H)-YL COMPOUNDS

Christopher David Beadle; David Andrew Coates; Junliang Hao; Jr. Joseph H. Krushinski; Matthew Robert Reinhard; John Mehnert Schaus; Craig Daniel Wolfangel


Archive | 2012

SUBSTITUTED [(5H-PYRROLO[2,1-c] [1,4]BENZODIAZEPIN-11-YL)PIPERAZIN-1-YL]-2,2-DIMETHYLPROPANOIC ACID COMPOUNDS AS DUAL ACTIVITY H1 INVERSE AGONISTS/5-HT2A ANTAGONISTS

Anne Marie Camp; Peter Thaddeus Gallagher; Andrew James Ledgard; Adam J. Sanderson; David Andrew Coates


Archive | 2017

TOSYLATE SALT OF N-[3-[(4AR,7AS)-2-AMINO-6-(5-FLUOROPYRIMIDIN-2-YL)-4,4A,5,7-TETRAHYDROPYRROLO[3,4-D][1,3]THIAZIN-7A-YL]-4-FLUORO-PHENYL]-5-METHOXY-PYRAZINE-2-CARBOXAMIDE

David Andrew Coates; Craig Daniel Wolfangel


Archive | 2017

métodos para aprimorar produção de galinha

Brian D. Burke; David Andrew Coates; Djamel Aissat; Jeffrey Glen Sherman


Archive | 2017

SAL DE TOSILATO DE N-[3-[(4AR,7AS)-2-AMINO-6-(5-FLUOROPIRIMIDINA-2-IL)-4,4A,5,7-TETRAHIDROPIRROLO[3,4-D][1,3]TIAZINA-7A-IL]-4-FLUORO-FENIL]-5-METOXI-PIRAZINA-2-CARBOXAMIDA

David Andrew Coates; Craig Daniel Wolfangel


Archive | 2016

SUBSTITUTED PHENYL IMIDAZOLYL PIPERIDYL COMPOUNDS AS P70S6K1 INHIBITORS

David Andrew Coates; Sajan Joseph; Craig Daniel Wolfangel


Archive | 2016

2-OXO-1,3,8-TRIAZASPIRO[4.5]DECAN-3-YL] CARBOXYLIC ACID DERIVATIVES

Thomas James Beauchamp; David Andrew Coates; Maria Angeles Martinez-Grau; Miguel A. Toledo

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