GPR40 reduces food intake and body weight through GLP-1

Gorski, Judith N.; Pachanski, Michele; Mane, Joel; Plummer, Christopher W.; Souza, Sarah; Thomas-Fowlkes, Brande; Ogawa, Aimie M.; Weinglass, Adam B.; Salvo, Jerry Di; Cheewatrakoolpong, Boonlert; Howard, Andrew D.; Colletti, Steven L.; Trujillo, María E.

doi:10.1152/ajpendo.00435.2016

Cited by 35 publications

(33 citation statements)

References 29 publications

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“…Further, these hormonal effects are observed alongside greater glucose lowering suggesting a possible causal link between these two observations. The data we described in this manuscript and others [ 5 , 23 ] extend these initial reports of greater efficacy with GPR40 AgoPAMs beyond what was first observed acutely in mice and cells to the chronic setting in the diabetic GK rat. Furthermore, these studies used two structurally distinct AgoPAM compounds dosed at levels aimed to achieve comparable percent target engagement as the partial GPR40 agonists used.…”

Section: Discussionsupporting

confidence: 79%

GPR40 partial agonists and AgoPAMs: Differentiating effects on glucose and hormonal secretions in the rodent

et al. 2017

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GPR40 agonists are effective antidiabetic agents believed to lower glucose through direct effects on the beta cell to increase glucose stimulated insulin secretion. However, not all GPR40 agonists are the same. Partial agonists lower glucose through direct effects on the pancreas, whereas GPR40 AgoPAMs may incorporate additional therapeutic effects through increases in insulinotrophic incretins secreted by the gut. Here we describe how GPR40 AgoPAMs stimulate both insulin and incretin secretion in vivo over time in diabetic GK rats. We also describe effects of AgoPAMs in vivo to lower glucose and body weight beyond what is seen with partial GPR40 agonists in both the acute and chronic setting. Further comparisons of the glucose lowering profile of AgoPAMs suggest these compounds may possess greater glucose control even in the presence of elevated glucagon secretion, an unexpected feature observed with both acute and chronic treatment with AgoPAMs. Together these studies highlight the complexity of GPR40 pharmacology and the potential additional benefits AgoPAMs may possess above partial agonists for the diabetic patient.

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Section: Discussionsupporting

confidence: 79%

GPR40 partial agonists and AgoPAMs: Differentiating effects on glucose and hormonal secretions in the rodent

et al. 2017

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“…These experiments also revealed the significance of blocking SSTR5. While combinations of just the DPP4 inhibitor and the TGR5 or GPR40 agonist increased GLP-1 concentrations (31 and 28 pmol/L, respectively; similar to levels reported for the DPP4 inhibitor-GPR40 agonist combination [39]), the addition of the SSTR5 Figure 2-Determining the concentration of GLP-1 equivalents that maximize glucose lowering. A: Wild-type mice fasted overnight were subcutaneously injected with exenatide (0.01-30 nmol/kg), followed 1 h later by assessment of exenatide levels in plasma (limit of detection of 24 pmol/L is denoted by the dotted line).…”

Section: Combination Therapy Elevates Active Glp-1 and Normalizes Possupporting

confidence: 52%

Mechanisms to Elevate Endogenous GLP-1 Beyond Injectable GLP-1 Analogs and Metabolic Surgery

Briere

Bueno

Gunn³

et al. 2017

Diabetes

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Therapeutic engineering of glucagon-like peptide 1 (GLP-1) has enabled development of new medicines to treat type 2 diabetes. These injectable analogs achieve robust glycemic control by increasing concentrations of "GLP-1 equivalents" (∼50 pmol/L). Similar levels of endogenous GLP-1 occur after gastric bypass surgery, and mechanistic studies indicate glucose lowering by these procedures is driven by GLP-1. Therefore, because of the remarkable signaling and secretory capacity of the GLP-1 system, we sought to discover mechanisms that increase GLP-1 pharmacologically. To study active GLP-1, glucose-dependent insulinotropic polypeptide receptor ()-deficient mice receiving background dipeptidyl peptidase 4 (DPP4) inhibitor treatment were characterized as a model for evaluating oral agents that increase circulating GLP-1. A somatostatin receptor 5 antagonist, which blunts inhibition of GLP-1 release, and agonists for TGR5 and GPR40, which stimulate GLP-1 secretion, were investigated alone and in combination with the DPP4 inhibitor sitagliptin; these only modestly increased GLP-1 (∼5-30 pmol/L). However, combining molecules to simultaneously intervene at multiple regulatory nodes synergistically elevated active GLP-1 to unprecedented concentrations (∼300-400 pmol/L), drastically reducing glucose in null and mice in a GLP-1 receptor-dependent manner. Our studies demonstrate that complementary pathways can be engaged to robustly increase GLP-1 without invasive surgical or injection regimens.

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“…Consistent with these results, the stimulatory effects of fatty acids on insulin secretion are lost in FFA1 receptor knockout mice (Lan et al ., ). Interestingly, a new report shows the ability of FFA1 receptor agonists or potentiators to increase GLP‐1 to levels sufficient for reducing food intake and body weight in obese rodents (Gorski et al ., ). Several FFA1 receptor agonists have entered clinical testing with mixed results.…”

Section: Why So Challenging: Lost In Translation From Mice To Men?mentioning

confidence: 97%

The current state of GPCR‐based drug discovery to treat metabolic disease

Sloop

Emmerson

Statnick

et al. 2018

British J Pharmacology

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GPR40 reduces food intake and body weight through GLP-1

Cited by 35 publications

References 29 publications

GPR40 partial agonists and AgoPAMs: Differentiating effects on glucose and hormonal secretions in the rodent

GPR40 partial agonists and AgoPAMs: Differentiating effects on glucose and hormonal secretions in the rodent

Mechanisms to Elevate Endogenous GLP-1 Beyond Injectable GLP-1 Analogs and Metabolic Surgery

The current state of GPCR‐based drug discovery to treat metabolic disease

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