Novel Use of Probenecid to Alleviate Symptoms of Opioid Withdrawal
NCT ID: NCT04939623
Last Updated: 2025-03-30
Study Results
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Basic Information
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RECRUITING
PHASE2
40 participants
INTERVENTIONAL
2023-10-31
2025-12-31
Brief Summary
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The investigators have recently explored the underlying causes of opioid withdrawal and identified an important target in the spinal cord that is responsible for producing withdrawal symptoms in rats and mice. The target, a protein called pannexin-1 (Panx1), is located throughout the body, specifically in the brain and spinal cord. Using sophisticated biochemical, genetic, and pharmacological techniques, the investigators demonstrated how Panx1 on immune cells is implicated in the production of opioid withdrawal symptoms after cessation of fentanyl and morphine in opioid dependent rodents. The investigators then attenuated these symptoms of withdrawal using probenecid, a drug which inherently blocks Panx1 activity. Because probenecid is a safe and clinically available drug, the findings could be immediately translated into clinical therapy to support people who are struggling with the symptoms of opioid withdrawal and provide clinicians with a safe and effective option for caring for this population.
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Detailed Description
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Our team has recently explored the underlying causes of opioid withdrawal and identified an important target in the spinal cord that is responsible for producing withdrawal symptoms in rats and mice. The target, a protein called pannexin-1 (Panx1), is located throughout the body, specifically in the brain and spinal cord. Using sophisticated biochemical, genetic, and pharmacological techniques, the investigators demonstrated how Panx1 on immune cells is implicated in the production of opioid withdrawal symptoms after cessation of fentanyl and morphine in opioid dependent rodents. The investigators then attenuated these symptoms of withdrawal using probenecid, a drug which inherently blocks Panx1 activity. Because probenecid is a safe and clinically available drug, the findings could be immediately translated into clinical therapy to support people who are struggling with the symptoms of opioid withdrawal and provide clinicians with a safe and effective option for caring for this population.
Probenecid was initially developed in the early 1950s as a tool to enhance the activity of penicillin and allow for outpatient treatment of various infections. It increases plasma levels and the half-life of weak organic acids (penicillins, cephalosporins, or other beta-lactam antibiotics) by competitively inhibiting their renal tubular secretion. As a result, it became widely used in combination with beta-lactam antibacterial agents. It is still occasionally used today in combination with cefazolin for the treatment of skin and soft tissue infections, and in combination with cefoxitin or doxycycline as an option for outpatient treatment of pelvic inflammatory disease.
Probenacid also competitively inhibits active reabsorption of uric acid at the level of the proximal convoluted tubule promoting excretion of uric acid, thereby reducing serum urate concentrations.
Probenecid is also used in combination with cidofovir for the prevention of cidofovir-related nephrotoxicity when used to treat cytomegalovirus retinitis in patients with HIV. More recently, the effects of probenecid on serotonin levels and TRPV2 channels has led to speculation about its utility in depression, Parkinson's Disease, and congestive heart failure.
The drug is no longer commercially available in Canada but is commercially available as 500 mg tablets in the United States which can be acquired through Health Canada's Special Access Program. Probenecid can, however, be prepared in Canada by compounding pharmacies.
The study is a single centre, randomized, double blind, placebo-controlled, 12-week clinical trial meant to study probenecid use among adult participants living with chronic non-cancer pain using opioid drug therapy on a daily basis and planning to voluntarily reduce their dose.
Conditions
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Study Design
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RANDOMIZED
PARALLEL
1. Probenecid 500 mg PO BID (16 participants)
2. Probenecid 1000 mg PO BID (16 participants)
3. Placebo PO BID (8 participants)
TREATMENT
TRIPLE
Study Groups
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Probenecid 500 mg PO BID
Probenecid 500 mg X 1 PO BID and Placebo X 1 PO BID
Probenecid
The Investigators aim to recruit 40 participants who will be followed for 12 weeks in duration. Participants will be randomized in a 2:2:1 ratio to one of probenecid 500 mg, 1000 mg, or placebo PO BID for 12 weeks. Justification for use of a non-active placebo comparator includes the fact that this trial is meant to identify tolerability and safety of probenecid in a population of patients living with chronic pain, this will be best measured by comparing to a non-active placebo.
Probenecid 1000 mg PO BID
Probenecid 500mg X 2 PO BID
Probenecid
The Investigators aim to recruit 40 participants who will be followed for 12 weeks in duration. Participants will be randomized in a 2:2:1 ratio to one of probenecid 500 mg, 1000 mg, or placebo PO BID for 12 weeks. Justification for use of a non-active placebo comparator includes the fact that this trial is meant to identify tolerability and safety of probenecid in a population of patients living with chronic pain, this will be best measured by comparing to a non-active placebo.
Placebo PO BID
Placebo X 2 PO BID
Probenecid
The Investigators aim to recruit 40 participants who will be followed for 12 weeks in duration. Participants will be randomized in a 2:2:1 ratio to one of probenecid 500 mg, 1000 mg, or placebo PO BID for 12 weeks. Justification for use of a non-active placebo comparator includes the fact that this trial is meant to identify tolerability and safety of probenecid in a population of patients living with chronic pain, this will be best measured by comparing to a non-active placebo.
Interventions
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Probenecid
The Investigators aim to recruit 40 participants who will be followed for 12 weeks in duration. Participants will be randomized in a 2:2:1 ratio to one of probenecid 500 mg, 1000 mg, or placebo PO BID for 12 weeks. Justification for use of a non-active placebo comparator includes the fact that this trial is meant to identify tolerability and safety of probenecid in a population of patients living with chronic pain, this will be best measured by comparing to a non-active placebo.
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
2. Subjects are currently taking a daily opioid pain medication and planning to taper the dose.
3. Participants complete at least one voluntary opioid dose reduction in the twelve-week study period.
4. Glomerular filtration rate (GFR) \> 50 mL/min
5. Capable of providing informed consent
Exclusion Criteria
2. History of uric acid renal calculi, if known to be urate calculi. If unknown type, then any history of renal calculi.
3. Known G6PD deficiency
4. Active gout in any joint
5. Current use of drugs whose exposure may be prolonged, or risk of toxicity increased when used in combination with probenecid:
1. Penicillins, specifically ampicillin, penicillin G sodium, and piperacillin
2. Carbapenems, specifically doripenem and meropenem
3. Lorazepam, midazolam, nitrazepam
4. Ketorolac
5. Oseltamivir
6. Methotrexate
7. Mycophenolate
6. Current use of drugs which may mask symptoms of withdrawal:
a. Clonidine, lofexidine, tizanidine
7. Current use of drugs which may diminish the effect of probenecid:
a. High dose salicylates including greater than 325 mg PO daily of acetylsalicylic acid (ASA)
8. Pregnancy or breastfeeding
9. Any major comorbid medical condition which might impair follow-up or result in a safety risk to the participant
10. Participation in another clinical trial investigating a drug, medical device, or a medical procedure during the 30 days prior to enrolment.
\-
18 Years
80 Years
ALL
No
Sponsors
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University of Calgary
OTHER
Responsible Party
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Principal Investigators
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Lori Montgomery, MD
Role: PRINCIPAL_INVESTIGATOR
University of Calgary
Locations
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Richmond Road Diagnostic and Treatment Centre
Calgary, Alberta, Canada
Countries
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Central Contacts
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Facility Contacts
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References
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1 Beyer, R. H., Wiebelhaus, V. D., Russe, H. F., Peck, H. M., & McKinney, S. E. (1950). Benemid: An anticatabolite; its phar- macological properties. Federation Proceedings, 9, 258.
Probenecid CPhA Monograph. RxTx. Date of Revision: November 2017. Accessed online at https://www.e-therapeutics.ca on February 21, 2018.
Robbins N, Koch SE, Tranter M, Rubinstein J. The history and future of probenecid. Cardiovasc Toxicol. 2012 Mar;12(1):1-9. doi: 10.1007/s12012-011-9145-8.
Benuryl Tablets, Probenecid Tablets. Prescribing Information. Montreal, Quebec. Valeant Canada LP. Date of Revision: September 1, 2004.
Related Links
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Probenecid CPhA Monograph. RxTx. Date of Revision: February 2014. Accessed online at https://www.e-therapeutics.ca on May 22, 2015.
Other Identifiers
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Probenacid 1.0
Identifier Type: -
Identifier Source: org_study_id
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