UG3DA059285
Cooperative Agreement
Overview
Grant Description
Development of CEBRANOPADOL, a potent dual MOP/NOP agonist, for the treatment of opioid use disorder (OUD) - Abstract/Summary
The U.S. is experiencing a crisis of opioid misuse, addiction, and overdose; in the most recent year, there were over 100,000 drug-related overdose deaths, 75% of which involved opioids.
Current pharmacotherapies for OUD target mu opioid peptide (MOP) receptors, one of five classes of opioid receptors. These therapies include the full MOP agonist methadone, the partial MOP agonist buprenorphine, and the MOP antagonist naltrexone.
There are several drawbacks in using these medications to treat OUD, which include the potential for abuse, development of physical dependence, and risk of overdose, particularly for methadone and buprenorphine. Buprenorphine and naltrexone also trigger severe withdrawal symptoms.
There is thus an urgent need for an improved therapeutic for the treatment of OUD.
CEBRANOPADOL (TRN-228) is a first-in-class synthetic drug developed for its dual-action mechanism in treating pain, mediated by high affinity and potency for both MOP and nociceptin/orphanin FQ receptor (NOP). NOP receptor activation has been associated with reduced development of tolerance, abuse-related behavior, addiction, and physical dependence.
In this UG3/UH3 proposal, Park Therapeutics is developing TRN-228 as a first-in-class dual MOP/NOP agonist that can be used as a safe and effective treatment for OUD.
Preliminary nonclinical and clinical data indicate that CEBRANOPADOL has low potential for abuse and physical dependence and produces milder respiratory depression compared to pure MOP agonists such as morphine and oxycodone. TRN-228 also decreases morphine, heroin, and cocaine self-administration in rats and did not induce withdrawal when given to opioid-dependent rats.
The UG3 phase of this proposal will test whether oral TRN-228 is a safe and potentially effective alternative treatment for OUD, based on the following specific aims:
1) Determining the effects of TRN-228 on intravenous fentanyl self-administration and fentanyl-induced respiratory depression in opioid-dependent rats.
2) Determining the IV abuse potential of TRN-228.
3) Assessing the ability of TRN-228 to suppress withdrawal.
Upon meeting the UG3 go/no-go milestones, Park will progress to the UH3 phase which will demonstrate the therapeutic efficacy of TRN-228 in decreasing opioid use with low risk of withdrawal or abuse, which will be accomplished by:
4) Determining the effects of TRN-228 on fentanyl-induced respiratory depression in opioid-tolerant participants.
5) Evaluating the ability of TRN-228 to block the subjective effects of hydromorphone.
These studies will significantly advance the field by establishing the safety and preliminary efficacy of TRN-228. Successful completion of these aims will guide future efforts to establish a clinical program for FDA approval.
The U.S. is experiencing a crisis of opioid misuse, addiction, and overdose; in the most recent year, there were over 100,000 drug-related overdose deaths, 75% of which involved opioids.
Current pharmacotherapies for OUD target mu opioid peptide (MOP) receptors, one of five classes of opioid receptors. These therapies include the full MOP agonist methadone, the partial MOP agonist buprenorphine, and the MOP antagonist naltrexone.
There are several drawbacks in using these medications to treat OUD, which include the potential for abuse, development of physical dependence, and risk of overdose, particularly for methadone and buprenorphine. Buprenorphine and naltrexone also trigger severe withdrawal symptoms.
There is thus an urgent need for an improved therapeutic for the treatment of OUD.
CEBRANOPADOL (TRN-228) is a first-in-class synthetic drug developed for its dual-action mechanism in treating pain, mediated by high affinity and potency for both MOP and nociceptin/orphanin FQ receptor (NOP). NOP receptor activation has been associated with reduced development of tolerance, abuse-related behavior, addiction, and physical dependence.
In this UG3/UH3 proposal, Park Therapeutics is developing TRN-228 as a first-in-class dual MOP/NOP agonist that can be used as a safe and effective treatment for OUD.
Preliminary nonclinical and clinical data indicate that CEBRANOPADOL has low potential for abuse and physical dependence and produces milder respiratory depression compared to pure MOP agonists such as morphine and oxycodone. TRN-228 also decreases morphine, heroin, and cocaine self-administration in rats and did not induce withdrawal when given to opioid-dependent rats.
The UG3 phase of this proposal will test whether oral TRN-228 is a safe and potentially effective alternative treatment for OUD, based on the following specific aims:
1) Determining the effects of TRN-228 on intravenous fentanyl self-administration and fentanyl-induced respiratory depression in opioid-dependent rats.
2) Determining the IV abuse potential of TRN-228.
3) Assessing the ability of TRN-228 to suppress withdrawal.
Upon meeting the UG3 go/no-go milestones, Park will progress to the UH3 phase which will demonstrate the therapeutic efficacy of TRN-228 in decreasing opioid use with low risk of withdrawal or abuse, which will be accomplished by:
4) Determining the effects of TRN-228 on fentanyl-induced respiratory depression in opioid-tolerant participants.
5) Evaluating the ability of TRN-228 to block the subjective effects of hydromorphone.
These studies will significantly advance the field by establishing the safety and preliminary efficacy of TRN-228. Successful completion of these aims will guide future efforts to establish a clinical program for FDA approval.
Awardee
Funding Goals
NOT APPLICABLE
Grant Program (CFDA)
Awarding / Funding Agency
Place of Performance
Monmouth Junction,
New Jersey
088523014
United States
Geographic Scope
Single Zip Code
Related Opportunity
Analysis Notes
Amendment Since initial award the total obligations have increased 100% from $3,329,591 to $6,654,182.
Park Therapeutics was awarded
Development of CEBRANOPADOL: A Dual MOP/NOP Agonist for Opioid Use
Cooperative Agreement UG3DA059285
worth $6,654,182
from National Institute on Drug Abuse in August 2023 with work to be completed primarily in Monmouth Junction New Jersey United States.
The grant
has a duration of 2 years and
was awarded through assistance program 93.279 Drug Abuse and Addiction Research Programs.
The Cooperative Agreement was awarded through grant opportunity Development of Medications to Prevent and Treat Opioid and/or Stimulant Use Disorders and Overdose (UG3/UH3 - Clinical Trial Optional).
Status
(Complete)
Last Modified 9/5/24
Period of Performance
8/15/23
Start Date
7/31/25
End Date
Funding Split
$6.7M
Federal Obligation
$0.0
Non-Federal Obligation
$6.7M
Total Obligated
Activity Timeline
Transaction History
Modifications to UG3DA059285
Additional Detail
Award ID FAIN
UG3DA059285
SAI Number
UG3DA059285-4272880290
Award ID URI
SAI UNAVAILABLE
Awardee Classifications
Small Business
Awarding Office
75N600 NIH NATIONAL INSITUTE ON DRUG ABUSE
Funding Office
75N600 NIH NATIONAL INSITUTE ON DRUG ABUSE
Awardee UEI
LKW7MCDM3GG5
Awardee CAGE
8TKS5
Performance District
NJ-12
Senators
Robert Menendez
Cory Booker
Cory Booker
Budget Funding
| Federal Account | Budget Subfunction | Object Class | Total | Percentage |
|---|---|---|---|---|
| National Institute on Drug Abuse, National Institutes of Health, Health and Human Services (075-0893) | Health research and training | Grants, subsidies, and contributions (41.0) | $3,329,591 | 100% |
Modified: 9/5/24