In vitro and in vivo assessment of the abuse potential of PF614, a novel BIO-MD™ prodrug of oxycodone

D Lynn Kirkpatrick; William K Schmidt; Ricardo Morales; John Cremin; Julie Seroogy; Craig Husfeld; Thomas Jenkins

doi:10.5055/jom.2017.0366

In vitro and in vivo assessment of the abuse potential of PF614, a novel BIO-MD™ prodrug of oxycodone

J Opioid Manag. 2017 Jan/Feb;13(1):39-49. doi: 10.5055/jom.2017.0366.

Authors

D Lynn Kirkpatrick¹, William K Schmidt², Ricardo Morales³, John Cremin³, Julie Seroogy³, Craig Husfeld³, Thomas Jenkins³

Affiliations

¹ CEO, Ensysce Biosciences Inc., San Diego, California.
² Ensysce Biosciences Inc., San Diego, California.
³ Signature Therapeutics Inc., Palo Alto, California.

PMID: 28345745
DOI: 10.5055/jom.2017.0366

Abstract

Objective: The need for pain medication which will not lead to abuse is well recognized. Ensysce has designed prodrug analogs of the commonly used pain medications including hydromorphone, oxycodone (OC), hydrocodone, and morphine that limit their use to oral delivery, two of which are in clinical development. This study was undertaken to demonstrate that PF614, an extended-release prodrug of OC, allows the release of OC as designed when delivered orally, yet it resists ex vivo extraction with household chemicals and is pharmacologically inactive when administered by nonoral routes (nasal and parenteral), thereby substantially reducing its intravenous (IV) and intranasal abuse potential.

Methods: In vitro and in vivo methods were used to determine release of OC from PF614 and to show potential µ-opioid receptor activity. Plasma and cerebral spinal fluid levels of OC were evaluated following in vivo IV administration of PF614 in rats. In vitro extraction of OC from PF614 was explored using enzymes, common solvents, and household chemicals at room temperature and elevated temperature over time to determine release of OC from the prodrug.

Results: PF614 was stable with in vitro exposure to human plasma, saliva, and liver microsomes or culinary enzyme preparations. PF614 was stable (≥90 percent remaining as intact prodrug) under all room temperature conditions evaluated for 24 hours. At 80°C for 1 hour, no OC was released. Incubation at 80°C for 24 hours in vinegar or vodka produced a conversion to OC of 6 percent. Incubation with trypsin at 37°C converted PF614 approximately stoichiometric to OC with half-life of 4 hours. PF614's penetration of the central nervous system was 83-fold lower than OC and it had a 6.5-fold reduced potency as a µ-opioid agonist. Finally, oral PF614 delivers OC into plasma with an extended-release profile in dogs (reduced C_max; delayed T_max).

Conclusions: The Bio-Activated Molecular Delivery prodrug design limits the use of PF614 to the intended oral route of delivery with reduced potential for IV or nasal abuse, as it cannot be activated intravenously or nasally to provide an active opioid. Unlike existing opioid formulations, the extended-release profile of PF614 cannot be accelerated by chewing or ex vivo extraction to pharmacologically active substances.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Analgesics, Opioid / administration & dosage
Analgesics, Opioid / adverse effects
Analgesics, Opioid / pharmacokinetics*
Animals
Binding Sites
Delayed-Action Preparations
Dogs
Drug Liberation
Drug Stability
Humans
Microsomes, Liver / metabolism
Opioid-Related Disorders / prevention & control*
Oxycodone / administration & dosage
Oxycodone / adverse effects
Oxycodone / pharmacokinetics*
Prodrugs / administration & dosage
Prodrugs / adverse effects
Prodrugs / pharmacokinetics*
Rats
Receptors, Opioid, mu / metabolism
Saliva / metabolism

Substances

Analgesics, Opioid
Delayed-Action Preparations
Prodrugs
Receptors, Opioid, mu
Oxycodone