A bitter pill for type 2 diabetes? The activation of bitter taste receptor TAS2R38 can stimulate GLP-1 release from enteroendocrine L-cells

Pham, Hung; Hui, Hongxiang; Morvaridi, Susan; Cai, Jiena; Zhang, San‐Qi; Tan, Jun; Wu, Vin‐Cent; Levin, Nancy; Knudsen, Beatrice S.; Goddard, William A.; Pandol, Stephen J.; Abrol, Ravinder

doi:10.1016/j.bbrc.2016.04.149

Cited by 46 publications

(42 citation statements)

References 39 publications

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“…Consistent with the role of BTR signaling in GLP-1 secretion, the effect of DB to slow gastric emptying was abolished by co-administration of probenecid ( 26 ). Similarly, intragastric administration of PTC has been reported to augment plasma GLP-1 concentrations ( 36 ) and slow gastric emptying ( 26 ) in mice. The latter effect was, however, not inhibited by probenecid ( 26 ).…”

Section: Effects Of Btr Signaling On Gut Hormone Secretionmentioning

confidence: 99%

“…Consistent with PCR observation, studies using double-labeling immunofluorescence have also shown co-localization of chromogranin A (a cellular marker of enteroendocrine cells) with T2Rs in the mouse small and large intestine ( 42 , 44 ). More specifically, co-expression of GLP-1 with various T2Rs in human enteroendocrine L cell lines (i.e., HuTu-80 and NCI-h716) and in small and large intestinal tissues has been observed ( 21 , 35 , 36 , 39 ). However, the co-expression of T2Rs with enteroendocrine cells containing other hormones is not well characterized in rodents or humans.…”

Section: Intestinal Bitter Taste Receptorsmentioning

confidence: 99%

“…For example, in both NCI-716 and STC-1 cells, berberine, a natural bitter plant alkaloid commonly used as an antibiotic, was shown to dose-dependently stimulate GLP-1 secretion via T2R38 ( 24 , 25 ). Similarly, a specific T2R38 agonist, phenylthiourea, induced GLP-1 secretion from HuTu-80 cells, an effect markedly inhibited by silencing of T2R38 with small interfering RNA ( 36 ), In contrast, 1,10-phenanthroline stimulates GLP-1 via T2R5 ( 39 ), and DB appears to induce GLP-1 secretion via a broad range of BTRs (including T2R4, T2R43, and T2R46 at least), in NCI-h716 cells ( 21 ). Furthermore, blockade of BTRs (e.g., by probenecid), or the downstream pathways relating to BTR signaling, including inositol 1,4,5-trisphophate, phospholipase C β 2 , protein kinase C and/or phosphodiesterase, attenuates GLP-1 secretion induced by bitter tastants ( 21 , 58 , 59 ).…”

Section: Effects Of Btr Signaling On Gut Hormone Secretionmentioning

confidence: 99%

“…In rodents, exposure of the gut to BTR agonists has also been shown to augment plasma GLP-1 levels ( 21 , 36 , 58 , 59 ). In acute settings, an intragastric preload of DB prior to enteral glucose administration increased plasma GLP-1 and insulin concentrations ( 21 ), slowed gastric emptying ( 26 , 65 ) and reduced blood glucose ( 21 ).…”

Section: Effects Of Btr Signaling On Gut Hormone Secretionmentioning

confidence: 99%

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Role of Intestinal Bitter Sensing in Enteroendocrine Hormone Secretion and Metabolic Control

et al. 2018

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The gastrointestinal tract stores ingested nutrients in the stomach which are then delivered to the small intestine at a controlled rate to optimize their digestion and absorption. The interaction of nutrients with the small and large intestine generates feedback that slows gastric emptying, induces satiation, and reduces postprandial glycemic excursions. The mechanisms underlying these nutrient-gut interactions are complex; it has only recently been appreciated that the gut has the capacity to detect intraluminal contents in much the same way as the tongue, via activation of specific G-protein-coupled receptors, and that ensuing signaling mechanisms modulate the release of an array of gut hormones that influence gastrointestinal motility, appetite and glycemia. Interestingly, evidence from preclinical models supports a functional link between intestinal bitter taste receptor (BTRs) and gastrointestinal hormone secretion, and the outcomes of recent studies indicate that stimulation of intestinal BTRs may be used to modulate gastrointestinal function, to diminish energy intake and limit postprandial blood glucose excursions in humans. This review summarizes current evidence about the expression and function of intestinal BTRs in relation to enteroendocrine hormone release and discusses the clinical implications of this pathway for the management of obesity and type 2 diabetes.

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Section: Effects Of Btr Signaling On Gut Hormone Secretionmentioning

confidence: 99%

Section: Intestinal Bitter Taste Receptorsmentioning

confidence: 99%

Section: Effects Of Btr Signaling On Gut Hormone Secretionmentioning

confidence: 99%

Section: Effects Of Btr Signaling On Gut Hormone Secretionmentioning

confidence: 99%

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Role of Intestinal Bitter Sensing in Enteroendocrine Hormone Secretion and Metabolic Control

et al. 2018

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“…STC-1 is originated from mouse duodenal tumours, while HuTu-80 is originated from a human duodenal adenocarcinoma. Both STC-1 and HuTu-80 cells are able to secrete GLP-1 upon nutrient stimulation, and are often used as cell models for studying GLP-1 secretion (Geraedts et al, 2011;Pham et al, 2016). However, GLP-1 secretion is not always similar among species (Kuhre et al, 2014) and cell lines (Kuhre et al, 2016).…”

Section: Introductionmentioning

confidence: 99%

Effect of food ingredients on glucagon‐like peptide‐1 secretion in STC‐1 and HuTu‐80 cells

Yue

Madsen

Hedemann

et al. 2019

Int J of Food Sci Tech

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Summary This study aims at identifying food ingredients that have potential to enhance satiety and therefore potentially can be used for preventing and treating obesity. To do so, effects of thirteen food ingredients on the secretion of gut satiety hormone glucagon‐like peptide‐1 (GLP‐1) in enteroendocrine STC‐1 and HuTu‐80 cells were investigated. First, the effects of food ingredients on cell viability were investigated. This was done to determine if the individual ingredient affected cell viability, and in case so, to determine the ingredient concentration below which, the cell viability was unaffected. Enzyme‐treated whey protein, palmitic acid, stearic acid, green tea extract, and hesperidin did not affect GLP‐1 secretion. Functional soy protein, fractionated functional soy protein, acetylated monoglyceride, N‐oleoylethanolamine, epigallocatechin‐3‐gallate, hesperetin, rosemary extract, and kale extract increased GLP‐1 secretion in at least one cell line. However, the effects of the eight potent ingredients on GLP‐1 secretion need to be further investigated in vivo.

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Humulus lupulus L.: Evaluation of Phytochemical Profile and Activation of Bitter Taste Receptors to Regulate Appetite and Satiety in Intestinal Secretin Tumor Cell Line (STC‐1 Cells)

Lela,

Carlucci,

Kioussi

et al. 2024

Molecular Nutrition Food Res

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ScopeInflorescences of the female hop plant (Humulus lupulus L.) contain biologically active compounds, most of which have a bitter taste. Given the rising global obesity rates, there is much increasing interest in bitter taste receptors (TAS2Rs). Intestinal TAS2Rs can have beneficial effects on obesity when activated by bitter agonists. This study aims to investigate the mechanism of action of a hydroalcoholic hop extract in promoting hormone secretion that reduces the sense of hunger at the intestinal level through the interaction with TAS2Rs.Methods and resultsThe results demonstrate that the hop extract is a rich source of bitter compounds (mainly α‐, β‐acids) that stimulate the secretion of anorexigenic peptides (glucagon‐like peptide 1 [GLP‐1], cholecystokinin [CCK]) in a calcium‐dependent manner while reducing levels of hunger‐related hormones like ghrelin. This effect is mediated through interaction with TAS2Rs, particularly Tas2r138 and Tas2r120, and through the activation of downstream signaling cascades. Knockdown of these receptors using siRNA transfection and inhibition of Trpm5, Plcβ‐2, and other calcium channels significantly reduces the hop‐induced calcium response as well as GLP‐1 and CCK secretion.ConclusionsThis study provides a potential application of H. lupulus extract for the formulation of food supplements with satiating activity capable of preventing or combating obesity.

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A bitter pill for type 2 diabetes? The activation of bitter taste receptor TAS2R38 can stimulate GLP-1 release from enteroendocrine L-cells

Cited by 46 publications

References 39 publications

Role of Intestinal Bitter Sensing in Enteroendocrine Hormone Secretion and Metabolic Control

Role of Intestinal Bitter Sensing in Enteroendocrine Hormone Secretion and Metabolic Control

Effect of food ingredients on glucagon‐like peptide‐1 secretion in STC‐1 and HuTu‐80 cells

Humulus lupulus L.: Evaluation of Phytochemical Profile and Activation of Bitter Taste Receptors to Regulate Appetite and Satiety in Intestinal Secretin Tumor Cell Line (STC‐1 Cells)

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