BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Lung cancer, Hippocampus, Anticancer prodrugs, Doxorubicin, rs7903146, DRD2)
Bookmark Forward

Dual allosteric modulation of opioid antinociceptive potency by α2A-adrenoceptors.

Anne-Julie Chabot-Doré, Magali Millecamps, Lina Naso, Dominic Devost, Phan Trieu, Marjo Piltonen, Luda Diatchenko, Carolyn A Fairbanks, George L Wilcox, Terence E Hébert, Laura S Stone

Neuropharmacology 2015 Dec


filter terms:
  • 2 receptor (4)
  • 6 ohda (1)
  • Adrenergic (4)
  • adrenoceptor (9)
  • analgesia (3)
  • antagonists opioid (1)
  • male (1)
  • mice (4)
  • mice knockout (1)
  • opioid (10)
  • opioid receptor (2)
  • pain (2)
  • spinal cord (2)
  • strain (1)
  • α2A AR (10)
    • Sizes of these terms reflect their relevance to your search.

    Opioid and α2-adrenoceptor (AR) agonists are analgesic when administered in the spinal cord and show a clinically beneficial synergistic interaction when co-administered. However, α2-AR antagonists can also inhibit opioid antinociception, suggesting a complex interaction between the two systems. The α2A-AR subtype is necessary for spinal adrenergic analgesia and synergy with opioids for most agonist combinations. Therefore, we investigated whether spinal opioid antinociception and opioid-adrenergic synergy were under allosteric control of the α2A-AR. Drugs were administered intrathecally in wild type (WT) and α2A-knock-out (KO) mice and antinociception was measured using the hot water tail immersion or substance P behavioral assays. The α2A-AR agonist clonidine was less effective in α2A-KO mice in both assays. The absence of the α2A-AR resulted in 10-70-fold increases in the antinociceptive potency of the opioid agonists morphine and DeltII. In contrast, neither morphine nor DeltII synergized with clonidine in α2A-KO mice, indicating that the α2AAR has both positive and negative modulatory effects on opioid antinociception. Depletion of descending adrenergic terminals with 6-OHDA resulted in a significant decrease in morphine efficacy in WT but not in α2A-KO mice, suggesting that endogenous norepinephrine acts through the α2A-AR to facilitate morphine antinociception. Based on these findings, we propose a model whereby ligand-occupied versus ligand-free α2A-AR produce distinct patterns of modulation of opioid receptor activation. In this model, agonist-occupied α2A-ARs potentiate opioid analgesia, while non-occupied α2A-ARs inhibit opioid analgesia. Exploiting such interactions between the two receptors could lead to the development of better pharmacological treatments for pain management. Copyright © 2015 Elsevier Ltd. All rights reserved.

    Citation

    Anne-Julie Chabot-Doré, Magali Millecamps, Lina Naso, Dominic Devost, Phan Trieu, Marjo Piltonen, Luda Diatchenko, Carolyn A Fairbanks, George L Wilcox, Terence E Hébert, Laura S Stone. Dual allosteric modulation of opioid antinociceptive potency by α2A-adrenoceptors. Neuropharmacology. 2015 Dec;99:285-300

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 26254859

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