Insights into the Role of Opioid Receptors in the GI Tract: Experimental Evidence and Therapeutic Relevance

Galligan, James J.; Sternini, Catia

doi:10.1007/164_2016_116

Cited by 90 publications

(106 citation statements)

References 82 publications

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“…5 Previous reports have indicated that the activation of these three opioid receptors is all associated with the inhibition of the acetylcholine and purine/nitric oxide release from the enteric neurons, causing gastrointestinal (GI) inhibition. 6 The MOP (eg, morphine and DAMGO) and DOP (eg, DPDLE) receptor agonists were reported to inhibit GI transit dose-dependently. 7 KOP receptor is expressed primarily in the myenteric plexus.…”

Section: Introductionmentioning

confidence: 99%

Central and peripheral modulation of gastrointestinal transit in mice by DN‐9, a multifunctional opioid/NPFF receptor agonist

Guo

Zhang

et al. 2020

Neurogastroenterology Motil

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Background The nonapeptide DN‐9 functions as a multifunctional agonist to opioid and neuropeptide FF (NPFF) receptors and exhibits antinociceptive effects at the central and peripheral levels. Methods The effects of DN‐9 on small and colonic intestinal transit were evaluated using the upper gastrointestinal (GI) transit test and colonic bead expulsion assay, respectively. Opioid and NPFF receptor antagonists were used to investigate the mechanisms of DN‐9‐induced GI inhibition. Furthermore, the agonism of the DN‐9 analog [Phg9]‐DN‐9 to opioid and NPFF receptors was tested by the cAMP assay. Key results Intracerebroventricular administration of DN‐9 dose‐dependently slowed upper GI transit and colonic expulsion via mu‐ and kappa‐opioid receptors in the brain, independent of the delta‐opioid receptor. Similarly, intraperitoneal injection of DN‐9 dose‐dependently inhibited GI propulsion via the peripheral opioid receptors. DN‐9‐induced GI transit inhibitions were significantly aggravated by the NPFF receptor antagonist RF9. Moreover, the DN‐9 analog [Phg9]‐DN‐9, an agonist at mu‐, delta‐, and kappa‐opioid receptors but not NPFF receptors, inhibited GI more potently than DN‐9. In addition, intracerebroventricular NPFF significantly attenuated the central inhibitory effects induced by [Phg9]‐DN‐9 and morphine. However, central and peripheral injections of NPFF or RF9 almost had no significant effects on GI transit by itself. Conclusion and Inferences Intracerebroventricular and intraperitoneal administrations of DN‐9 inhibit GI transit via opioid receptors in mice by central and peripheral mechanisms, respectively. In addition, the NPFF agonism of DN‐9 possesses antiopioid effects on GI transit, which might explain the reduced constipation at the antinociceptive doses.

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Section: Introductionmentioning

confidence: 99%

Central and peripheral modulation of gastrointestinal transit in mice by DN‐9, a multifunctional opioid/NPFF receptor agonist

Guo

Zhang

et al. 2020

Neurogastroenterology Motil

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“…Lembo et al showed that the μ‐opioid agonist, fentanyl, inhibits the perception of phasic rectal distention in a dose‐dependent fashion. In addition, activation of μ and δ opioid receptors reduces active Cl − secretion and passive water movement into the colonic lumen by inhibiting submucosal secretomotor neurons, which can result in stool of more solid consistency …”

Section: Introductionmentioning

confidence: 99%

“…In addition, activation of μ and δ opioid receptors reduces active Cl − secretion and passive water movement into the colonic lumen by inhibiting submucosal secretomotor neurons, which can result in stool of more solid consistency. 11 Peripherally active μ-opioid receptor antagonists (PAMORA) have emerged as a treatment option for chronic opioid-induced constipation (OIC). 12 Naloxegol is a novel PAMORA which is efficacious in the treatment of chronic OIC when administered orally at a dose of 25 mg daily.…”

Section: Introductionmentioning

confidence: 99%

Effects of naloxegol on whole gut transit in opioid‐naïve healthy subjects receiving codeine: A randomized, controlled trial

Halawi

Vijayvargiya

Busciglio

et al. 2018

Neurogastroenterology Motil

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“…This idea is supported by our findings that both TMEM16A inhibitor and loperamide delay gastric emptying, whereas only loperamide slowed whole-gut transit. Opioids have multiple actions on gut, including inhibition of ICCs by activating K + -ATP channels and suppression of enteric neurons and intestinal secretion, which indirectly inhibits stretch-induced motility (30). Because TMEM16A is not expressed in enterocytes or enteric neurons, TMEM16A inhibition is not expected to affect the determinants of gut motility other than ICC activity.…”

Section: Discussionmentioning

confidence: 99%

“…Mice were administered TM inh -23 at 10 mg/kg (in saline containing 5% DMSO and 10% Kolliphor HS 15) either intraperitoneally or by oral gavage. Blood samples were collected at 15,30,60,120, and 240 min by orbital puncture and centrifuged at 5000 rpm for 15 min at 25°C to separate serum. Solid-phase extraction columns (C18, HyperSep 60108-304; Thermo Fisher Scientific, Waltham, MA, USA) were conditioned with methanol (2 ml) followed by PBS (2 ml).…”

Section: Pharmacokineticsmentioning

confidence: 99%

Slowed gastric emptying and improved oral glucose tolerance produced by a nanomolar‐potency inhibitor of calcium‐activated chloride channel TMEM16A

Çil¹,

Anderson²,

Yen³

et al. 2019

FASEB j.

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Interstitial cells of Cajal, which express the calcium‐activated chloride channel transmembrane member 16A (TMEM16A), are an important determinant of gastrointestinal (GI) motility. We previously identified the acylaminocycloalkylthiophene class of TMEM16A inhibitors, which, following medicinal chemistry, gave analog 2‐bromodifluoroacetylamino‐5,6,7,8‐tetrahydro‐4H‐cyclohepta[b]thiophene‐3‐carboxylic acid o‐tolylamide (TMinh‐23) with 30 nM half‐maximal inhibitory concentration. Here, we tested the efficacy of TMinh‐23 for inhibition of GI motility in mice. In isolated murine gastric antrum, TMinh‐23 strongly inhibited spontaneous and carbachol‐stimulated rhythmic contractions. Pharmacokinetic analysis showed predicted therapeutic concentrations of TMinh‐23 for at least 4 h following a single oral or intraperitoneal dose at 10 mg/kg. Gastric emptying, as assessed following an oral bolus of phenol red or independently by [99mTc]‐diethylenetriamine pentaacetic acid scintigraphy, was reduced by TMinh‐23 by ∼60% at 20 min. Interestingly, there was little effect of TMinh‐23 on baseline whole‐gut transit time or time to diarrhea induced by castor oil. Consequent to the delay in gastric emptying, TMinh‐23 administration significantly reduced the elevation in blood sugar in mice following an oral but not intraperitoneal glucose load. These results provide pharmacological evidence for involvement of TMEM16A in gastric emptying and suggest the utility of TMEM16A inhibition in disorders of accelerated gastric emptying, such as dumping syndrome, and potentially for improving glucose tolerance in diabetes mellitus/metabolic syndrome and enhancing satiety in obesity.—Cil, O., Anderson, M. O., Yen, R., Kelleher, B., Huynh, T. L., Seo, Y., Nilsen, S. P., Turner, J. R., Verkman, A. S. Slowed gastric emptying and improved oral glucose tolerance produced by a nanomolar‐potency inhibitor of calcium‐activated chloride channel TMEM16A. FASEB J. 33, 11247–11257 (2019). http://www.fasebj.org

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Insights into the Role of Opioid Receptors in the GI Tract: Experimental Evidence and Therapeutic Relevance

Cited by 90 publications

References 82 publications

Central and peripheral modulation of gastrointestinal transit in mice by DN‐9, a multifunctional opioid/NPFF receptor agonist

Central and peripheral modulation of gastrointestinal transit in mice by DN‐9, a multifunctional opioid/NPFF receptor agonist

Effects of naloxegol on whole gut transit in opioid‐naïve healthy subjects receiving codeine: A randomized, controlled trial

Slowed gastric emptying and improved oral glucose tolerance produced by a nanomolar‐potency inhibitor of calcium‐activated chloride channel TMEM16A

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