Nalbuphine Potentiates Reversal of Fentanyl Overdose by Naloxone

Author:

Cernea Mihai1ORCID,Nikonov Georgiy2,Ataiants Janna3,Ştefănuţ Cristina1ORCID,Abernethy John4,Voronkov Michael2ORCID

Affiliation:

1. Department of Pharmacology, Faculty of Veterinary Medicine, University of Agricultural Sciences and Veterinary Medicine, 400372 Cluj-Napoca, Romania

2. Κappa Pharmaceuticals LLC, Alachua, FL 32615, USA

3. Dornsife School of Public Health, Drexel University, Philadelphia, PA 19104, USA

4. Serodopa Therapeutics Inc., Gainesville, FL 32601, USA

Abstract

Developing an effective antidote for fentanyl-induced overdose to achieve timely reversal is an unmet public health need. Previously, we found that naloxone derivative NX90 with mild κ-opioid agonistic properties was three-fold more effective than the parent naloxone in reversing a fentanyl overdose in rats. To investigate whether κ-agonistic properties could indeed augment the robustness of overdose reversal, we evaluated a κ-agonist/µ-antagonist nalbuphine (NB) as well as its combinations with naloxone (NX) in a fentanyl overdose model in rodents. An administration of either NB or NX as single agents at 0.1 mg/kg doses produced a full recovery in 90 ± 9.9 min and 11.4 ± 2.7 min, respectively. A higher dose of NX at 0.2 mg/kg reversed an overdose within 4.8 ± 1.0 min. In contrast to that, the coadministration of NB and NX at 0.1 mg/kg each produced a synergistic effect, with overdose reversal in 3.4 ± 0.2 min. The coadministration of NX and NB at sub-therapeutic doses of 0.05 mg/kg each was also 1.2-fold more effective than NX at 0.2 mg/kg. We further found that co-administration of NB at different doses (0.025, 0.05, 0.1 mg/kg) and ratios (1:4 and 1:1) with NX had differential effects on overdose reversal, cardiorespiratory liabilities, and analgesia.

Funder

Κappa Pharmaceuticals, LLC

Serodopa Therapeutics, Inc.

Publisher

MDPI AG

Reference37 articles.

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