Glucose sensing and signalling; regulation of intestinal glucose transport

Shirazi-Beechey, Soraya P.; Moran, Andrew W.; Batchelor, Daniel J.; Daly, Kristian; Al-Rammahi, Miran

doi:10.1017/s0029665111000103

Cited by 120 publications

(94 citation statements)

References 81 publications

(137 reference statements)

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“…Our present findings implicating regulation of the colonic SCFA transporter MCT1 via nutrient sensing are of considerable interest because, despite the fact that colonic luminal SCFA levels vary significantly depending upon dietary composition, gut microbiota, and disease, a SCFA-sensing mechanism regulating colonic luminal SCFA absorption has not been described previously. In recent years, the importance of cell surface receptors in nutrient sensing has increasingly been recognized (21,29). For example, recent discovery of the expression of T1R sweet taste receptor families on the apical membranes of enterocytes suggested that activities of these receptors might underlie the mechanisms of enhanced glucose absorption via increased apical membrane insertion of Glut2 after a meal (21).…”

Section: Discussionmentioning

confidence: 99%

A novel nutrient sensing mechanism underlies substrate-induced regulation of monocarboxylate transporter-1

Borthakur

Priyamvada

Kumar

et al. 2012

American Journal of Physiology-Gastrointestinal and Liver Physi

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A novel nutrient sensing mechanism underlies substrate-induced regulation of monocarboxylate transporter-1. Am J Physiol Gastrointest Liver Physiol 303: G1126 -G1133, 2012. First published September 12, 2012 doi:10.1152/ajpgi.00308.2012.-Monocarboxylate transporter isoform-1 (MCT1) plays an important role in the absorption of short-chain fatty acids (SCFAs) in the colon. Butyrate, a major SCFA, serves as the primary energy source for the colonic mucosa, maintains epithelial integrity, and ameliorates intestinal inflammation. Previous studies have shown substrate (butyrate)-induced upregulation of MCT1 expression and function via transcriptional mechanisms. The present studies provide evidence that shortterm MCT1 regulation by substrates could be mediated via a novel nutrient sensing mechanism. Short-term regulation of MCT1 by butyrate was examined in vitro in human intestinal C2BBe1 and rat intestinal IEC-6 cells and ex vivo in rat intestinal mucosa. Effects of pectin feeding on MCT1, in vivo, were determined in rat model. Butyrate treatment (30 -120 min) of C2BBe1 cells increased MCT1 function {p-(chloromercuri) benzene sulfonate (PCMBS)-sensitive [ 14 C]butyrate uptake} in a pertussis toxin-sensitive manner. The effects were associated with decreased intracellular cAMP levels, increased V max of butyrate uptake, and GPR109A-dependent increase in apical membrane MCT1 level. Nicotinic acid, an agonist for the SCFA receptor GPR109A, also increased MCT1 function and decreased intracellular cAMP. Pectin feeding increased apical membrane MCT1 levels and nicotinate-induced transepithelial butyrate flux in rat colon. Our data provide strong evidence for substrateinduced enhancement of MCT1 surface expression and function via a novel nutrient sensing mechanism involving GPR109A as a SCFA sensor. SCFA absorption; cyclic AMP; GPR109A SHORT-CHAIN FATTY ACIDS (SCFAs) acetate, propionate, and butyrate are produced in the colonic lumen by bacterial fermentation of dietary fiber. Of these SCFAs, butyrate plays a prominent role to serve as primary fuel for the colonocytes, and its oxidation is critical to various important metabolic processes in the colon (7). It is believed that a major consequence of reduction in intracellular SCFA oxidation results in metabolic starvation and mucosal atrophy (7). Besides its role as energy nutrient, butyrate is also vital in maintaining health and integrity of colonic mucosa by virtue of its multiple beneficial effects (4, 12, 22), such as its ability to improve barrier function and ameliorate intestinal inflammation. However, the ability of butyrate to exert many of these cellular effects is concentration dependent and the absorption of luminal butyrate is critical for the health benefits it confers to the intestinal mucosa (33, 34).We and others have shown that monocarboxylate transporter-1 (MCT1) plays an important role in the absorption of luminal SCFAs by the colonocytes (11, 28). Despite controversies regarding apical versus basolateral localization of MCT1 in various species (9,14),...

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Section: Discussionmentioning

confidence: 99%

A novel nutrient sensing mechanism underlies substrate-induced regulation of monocarboxylate transporter-1

Borthakur

Priyamvada

Kumar

et al. 2012

American Journal of Physiology-Gastrointestinal and Liver Physi

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“…In turn, there is an induction and functional activation of the glucose transporter SGLT1 [100]. Although the induction of SGLT1 is mediated through GLP-2, the GLP-2 receptor is on submucosal neurons, not on the epithelium, which implies that the increased glucose transport is a nerve-mediated effect [103]. GLP-2 excites submucosal neurons [104].…”

Section: Motor Neuron Influence On the Glucose Transportermentioning

confidence: 99%

The Enteric Nervous System and Gastrointestinal Innervation: Integrated Local and Central Control

Furness

Callaghan

Rivera

et al. 2014

Advances in Experimental Medicine and Biology

655

648

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The digestive system is innervated through its connections with the central nervous system (CNS) and by the enteric nervous system (ENS) within the wall of the gastrointestinal tract. The ENS works in concert with CNS reflex and command centers and with neural pathways that pass through sympathetic ganglia to control digestive function. There is bidirectional information flow between the ENS and CNS and between the ENS and sympathetic prevertebral ganglia.The ENS in human contains 200-600 million neurons, distributed in many thousands of small ganglia, the great majority of which are found in two plexuses, the myenteric and submucosal plexuses. The myenteric plexus forms a continuous network that extends from the upper esophagus to the internal anal sphincter. Submucosal ganglia and connecting fiber bundles form plexuses in the small and large intestines, but not in the stomach and esophagus. The connections between the ENS and CNS are carried by the vagus and pelvic nerves and sympathetic pathways. Neurons also project from the ENS to prevertebral ganglia, the gallbladder, pancreas and trachea.The relative roles of the ENS and CNS differ considerably along the digestive tract. Movements of the striated muscle esophagus are determined by neural pattern generators in the CNS. Likewise the CNS has a major role in monitoring the state of the stomach and, in turn, controlling its contractile activity and acid secretion, through vago-vagal reflexes. In contrast, the ENS in the small intestine and colon contains full reflex circuits, including sensory neurons, interneurons and several classes of motor neuron, through which muscle activity, transmucosal fluid fluxes, local blood flow and other functions are controlled. The CNS has control of defecation, via the defecation centers in the lumbosacral spinal cord. The importance of the ENS is emphasized by the life-threatening effects of some ENS neuropathies. By contrast, removal of vagal or sympathetic connections with the gastrointestinal tract has minor effects on GI function. Voluntary control of defecation is exerted through pelvic connections, but cutting these connections is not life-threatening and other functions are little affected.

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“…It may be that postabsorptive glucose actions can reinforce flavor preferences when there is also preabsorptive nutrient stimulation as provided by the flavored chow used in the Tordoff and Friedman study. Currently, there is considerable interest in the role of intestinal T1R2ϩT1R3 sweet receptors in carbohydrate absorption and hormone release (19,55), but these gut receptors are not implicated in sugar-stimulated intake or flavor conditioning. In particular, the failure of fructose to stimulate drinking in experiment 1 and the relatively weak flavor conditioning effect of IG fructose observed in other studies (4,46,47) argues against the involvement of intestinal sweet receptors, because fructose is a potent sweet receptor ligand.…”

Section: Glucose Stimulated Intakementioning

confidence: 99%

Rapid post-oral stimulation of intake and flavor conditioning by glucose and fat in the mouse

Zukerman

Ackroff

Sclafani

2011

American Journal of Physiology-Regulatory, Integrative and Comp

108

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-Although widely assumed to have only satiating actions, nutrients in the gut can also condition increases in intake in some cases. Here we studied the time course of post-oral nutrient stimulation of ingestion in food-restricted C57BL/6J mice. In experiment 1, mice adapted to drink a 0.8% sucralose solution 1 h/day, rapidly increased their rate of licking (within 4 -6 min) when first tested with an 8% glucose solution and even more so in tests 2 and 3. Other mice decreased their licking rate when switched from sucralose to 8% fructose, a sugar that is sweet like glucose but lacks positive post-oral effects in mice. The glucose-stimulated drinking is due to the sugar's post-oral rather than taste properties, because sucralose is highly preferred to glucose and fructose in brief choice tests. A second experiment showed that the glucose-stimulated ingestion is associated with a conditioned flavor preference in both intact and capsaicin-treated mice. This indicates that the post-oral stimulatory action of glucose is not mediated by capsaicin-sensitive visceral afferents. In experiment 3, mice consumed flavored saccharin solutions as they self-infused water or glucose via an intragastric (IG) catheter. The glucose self-infusion stimulated ingestion within 13-15 min in test 1 and produced a conditioned increase in licking that was apparent in the initial minute of tests 2 and 3. Experiment 4 revealed that IG self-infusions of a fat emulsion also resulted in post-oral stimulation of licking in test 1 and conditioned increases in tests 2 and 3. These findings indicate that glucose and fat can generate stimulatory post-oral signals early in a feeding session that increase ongoing ingestion and condition increases in flavor acceptance and preference revealed in subsequent feeding sessions. The test procedures developed here can be used to investigate the peripheral and central processes involved in stimulation of intake by post-oral nutrients.conditioned flavor acceptance and preference; fructose; sucralose; capsaicin deafferentation; intragastric infusion THE OROSENSORY AND POST-ORAL nutritional properties of foods are important determinants of food intake and preference. The flavors of palatable foods, i.e., their taste, odor, and texture, stimulate feeding, whereas post-oral signals are often assumed to have only inhibitory action via satiation signals that terminate a feeding bout and satiety signals that suppress postmeal eating (10,24,56). However, there is extensive evidence that nutrients can have other post-oral effects that condition food preferences and, in some cases, increase intake (42). This has been demonstrated, for example, by studies in which rodents are trained to drink a flavored nonnutritive solution paired with intragastric (IG) self-infusion of a nutrient. Typically, animals are given multiple training trials with one flavor (the conditioned stimulus or CSϩ) paired with a concurrent IG nutrient self-infusion and a second flavor (CSϪ) paired with IG water self-infusion on alternate training days. T...

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Glucose sensing and signalling; regulation of intestinal glucose transport

Cited by 120 publications

References 81 publications

A novel nutrient sensing mechanism underlies substrate-induced regulation of monocarboxylate transporter-1

A novel nutrient sensing mechanism underlies substrate-induced regulation of monocarboxylate transporter-1

The Enteric Nervous System and Gastrointestinal Innervation: Integrated Local and Central Control

Rapid post-oral stimulation of intake and flavor conditioning by glucose and fat in the mouse

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