BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. DRD2, nitric oxide metabolic process, Inflammatory disorder, Breast, Neocentromeres)
Bookmark Forward

AM841, a covalent cannabinoid ligand, powerfully slows gastrointestinal motility in normal and stressed mice in a peripherally restricted manner.

C M Keenan, M A Storr, G A Thakur, J T Wood, J Wager-Miller, A Straiker, M R Eno, S P Nikas, M Bashashati, H Hu, K Mackie, A Makriyannis, K A Sharkey

British journal of pharmacology 2015 May


filter terms:
  • am841 (8)
  • analgesia (2)
  • brain (2)
  • CA1 (1)
  • CA2 (1)
  • CA3 (1)
  • cannabinoid (3)
  • cannabinoid receptor (4)
  • cannabinoid receptor (2)
  • CB1 (1)
  • cells (1)
  • Cnr2 (1)
  • dronabinol (2)
  • hypothermia (3)
  • intestine (3)
  • ligand (8)
  • male (1)
  • mice (3)
  • mice knockout (1)
  • motor activity (1)
  • nervous system (1)
  • neurons (1)
  • pain (1)
  • pain threshold (1)
  • receptor (2)
  • receptor cannabinoid, cb1 (3)
  • receptor cannabinoid, cb1 (2)
  • receptor cannabinoid, cb2 (2)
  • region (3)
  • small intestine (2)
  • time factors (1)
  • treatment pain (1)
  • vitro (2)
    • Sizes of these terms reflect their relevance to your search.

    Cannabinoid (CB) ligands have been demonstrated to have utility as novel therapeutic agents for the treatment of pain, metabolic conditions and gastrointestinal (GI) disorders. However, many of these ligands are centrally active, which limits their usefulness. Here, we examine a unique novel covalent CB receptor ligand, AM841, to assess its potential for use in physiological and pathophysiological in vivo studies. The covalent nature of AM841 was determined in vitro using electrophysiological and receptor internalization studies on isolated cultured hippocampal neurons. Mouse models were used for behavioural analysis of analgesia, hypothermia and hypolocomotion. The motility of the small and large intestine was assessed in vivo under normal conditions and after acute stress. The brain penetration of AM841 was also determined. AM841 behaved as an irreversible CB1 receptor agonist in vitro. AM841 potently reduced GI motility through an action on CB1 receptors in the small and large intestine under physiological conditions. AM841 was even more potent under conditions of acute stress and was shown to normalize accelerated GI motility under these conditions. This compound behaved as a peripherally restricted ligand, showing very little brain penetration and no characteristic centrally mediated CB1 receptor-mediated effects (analgesia, hypothermia or hypolocomotion). AM841, a novel peripherally restricted covalent CB1 receptor ligand that was shown to be remarkably potent, represents a new class of potential therapeutic agents for the treatment of functional GI disorders. © 2015 The British Pharmacological Society.

    Citation

    C M Keenan, M A Storr, G A Thakur, J T Wood, J Wager-Miller, A Straiker, M R Eno, S P Nikas, M Bashashati, H Hu, K Mackie, A Makriyannis, K A Sharkey. AM841, a covalent cannabinoid ligand, powerfully slows gastrointestinal motility in normal and stressed mice in a peripherally restricted manner. British journal of pharmacology. 2015 May;172(9):2406-18

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 25572435

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.