4.7 Article

Mitragynine/Corynantheidine Pseudoindoxyls As Opioid Analgesics with Mu Agonism and Delta Antagonism, Which Do Not Recruit β-Arrestin-2

Journal

JOURNAL OF MEDICINAL CHEMISTRY
Volume 59, Issue 18, Pages 8381-8397

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.jmedchem.6b00748

Keywords

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Funding

  1. National Institute on Drug Abuse [DA034106]
  2. Harrington Discovery Institute Scholar Award
  3. Peter F. McManus Charitable Trust [DA013997, DA02944]
  4. National Science Foundation Graduate Research Fellowship [DGE-1257284]
  5. State of Florida, Executive Office of the Governor's Office of Tourism, Trade, and Economic Development
  6. NIH/NCI Cancer Center Support Grant [P30 CA008748]
  7. Janos Bolyai Research Fellowship

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Natural products found in Mitragyna speciosa, commonly known as kratom, represent diverse scaffolds (indole, indolenine, and spiro pseudoindoxyl) with opioid activity, providing opportunities to better understand opioid pharmacology. Herein, we report the pharmacology and SAR studies both in vitro and in vivo of mitragynine pseudoindoxyl (3), an oxidative rearrangement product of the corynanthe alkaloid mitragynine. 3 and its corresponding corynantheidine analogs show promise as potent analgesics with a mechanism of action that includes mu opioid receptor agonism/delta opioid receptor antagonism. In vitro, 3 and its analogs were potent agonists in [S-35]GTP gamma S assays at the mu opioid receptor but failed to recruit beta-arrestin-2, which is associated with opioid side effects. Additionally, 3 developed analgesic tolerance more slowly than morphine, showed limited physical dependence, respiratory depression, constipation, and displayed no reward or aversion in CPP/CPA assays, suggesting that analogs might represent a promising new generation of novel pain relievers.

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