Biasing Gβγ Downstream Signaling with Gallein Inhibits Development of Morphine Tolerance and Potentiates Morphine-Induced nociception in a Tolerant State

Gissell A Sanchez; Alan V Smrcka; Emily M Jutkiewicz

doi:10.1124/molpharm.124.000875

Biasing Gβγ Downstream Signaling with Gallein Inhibits Development of Morphine Tolerance and Potentiates Morphine-Induced nociception in a Tolerant State

Mol Pharmacol. 2024 May 31:MOLPHARM-AR-2024-000875. doi: 10.1124/molpharm.124.000875. Online ahead of print.

Authors

Gissell A Sanchez¹, Alan V Smrcka², Emily M Jutkiewicz³

Affiliations

¹ Pharmacology, University of Michigan, United States.
² Dept of Pharmacology, University of Michigan Medical School, United States avsmrcka@umich.edu.
³ Pharmacology, University of Michigan, United States ejutkiew@umich.edu.

PMID: 38769020
DOI: 10.1124/molpharm.124.000875

Abstract

Opioid analgesics are widely used as a treatment option for pain management and relief. However, the misuse of opioid analgesics has contributed to the current opioid epidemic in the United States. Prescribed opioids such as morphine, codeine, oxycodone, and fentanyl are mu-opioid receptor (MOR) agonists primarily used in the clinic to treat pain or during medical procedures, but development of tolerance limits their utility for treatment of chronic pain. Here we explored the effects of biasing Gβγ-signaling on tolerance development following chronic morphine treatment in vivo We hypothesized that biasing Gβγ-signaling with gallein could prevent activation of regulatory signaling pathways that result in tolerance to antinociceptive effects of MOR agonists. Gallein has been shown to bind to Gβγ and inhibit interactions of Gβγ with PLCβ3 or GRK2 but not GIRK channels. In mice, morphine-induced antinociception was evaluated in the 55{degree sign}C warm water tail withdrawal assay. We used two paradigms for gallein treatment: administration during and after 3x daily morphine administration. Our results show that gallein cotreatment during repeated administration of morphine decreased opioid tolerance development, and gallein treatment in an opioid-tolerant state enhanced the potency of morphine. Mechanistically, our data suggest that PLCβ3 is necessary for potentiating effects of gallein in an opioid-tolerant state but not in preventing the development of tolerance. These studies demonstrate that small molecules that target Gβγ-signaling could reduce the need for large doses of opioid analgesics to treat pain by producing an opioid-sparing effect. Significance Statement Biasing Gβγ-signaling prevents tolerance to repeated morphine administration in vivo and potentiates the antinociceptive effects of morphine in an opioid-tolerant state. Mechanistically, PLCβ is necessary for potentiating effects of gallein in an opioid-tolerant state but not in preventing the development of tolerance. This study identifies a novel treatment strategy to decrease the development of tolerance to the analgesic effects of MOR agonists, which are necessary to improve pain treatment and decrease the incidence of OUD.

Keywords: G proteins; behavior; opioid receptors.