Using Tezampanel to treat opioid withdrawal in patients with opioid use disorder
A Phase I, Single-Center, Single-Blind, Placebo-Controlled, Dose-Escalation Study to Assess the Safety, Pharmacokinetics and Efficacy of Tezampanel for Opioid Withdrawal Syndrome in Treatment-Seeking Patients With Opioid Use Disorder
This study is testing if a new medication called Tezampanel can help people with opioid use disorder feel better during withdrawal.
Quick facts
| Phase | Phase 1 |
|---|---|
| Study type | Interventional |
| Enrollment | 40 (estimated) |
| Ages | 18 Years to 65 Years |
| Sex | All |
| Sponsor | Proniras Corporation Industry-sponsored |
| Locations | 1 site (Indianapolis, Indiana) |
| Trial ID | NCT06538558 on ClinicalTrials.gov |
What this trial studies
This study examines the effectiveness of Tezampanel (TZP) in treating Opioid Withdrawal Syndrome (OWS) in individuals diagnosed with Opioid Use Disorder (OUD). Participants will be enrolled in a 7-day inpatient program where they will receive either TZP or a placebo daily from Days 2 to 7. The study aims to assess the safety, pharmacokinetics, and efficacy of TZP in alleviating withdrawal symptoms. It is a phase I, single-center, single-blind, dose escalation study involving four cohorts of treatment-seeking patients.
Who should consider this trial
Good fit: Ideal candidates are adults aged 18 to 65 with a diagnosis of opioid use disorder who are actively engaged in an outpatient treatment program.
Not a fit: Patients who are not currently seeking treatment for opioid use disorder or those who do not meet the inclusion criteria may not benefit from this study.
Why it matters
Potential benefit: If successful, this treatment could significantly improve the management of opioid withdrawal symptoms, aiding recovery for patients with opioid use disorder.
How similar studies have performed: While there have been studies on various treatments for opioid withdrawal, the specific use of Tezampanel for this purpose is novel and has not been extensively tested.
Eligibility criteria
Show full inclusion / exclusion criteria
Inclusion Criteria: 1. Male, female or non-binary, age 18 to 65 years of age at Screening. 2. Diagnosis of Opioid Use Disorder (OUD) 3. Positive Urine Drug Screen (UDS) for opioid(s) at the Screening and Baseline Visits. 4. Recent active/chronic use of short-acting illicit and/or prescribed opioids and/or long-acting Opioid Use Disorder (OUD) maintenance treatments buprenorphine or methadone at the Screening and Baseline Visits. 5. Already engaged and fully assessed in a longitudinal-outpatient treatment program that provides opioid addiction treatment encompassing the full spectrum of opioid maintenance and abstinence (injectable Vivitrol®) treatments, in which the host clinic is prepared and equipped to continue with: 1. maintenance treatment (methadone or buprenorphine treatment) for study non-completers, or 2. long-acting injectable naltrexone treatment (Vivitrol®), for completers with next dose delivered approximately 30 days after Study Day 6. 6. Post-menopausal/sterile or agree to use chemical or barrier methods of birth control from time of informed consent through 30 days post last treatment. 7. Stable concomitant medications. 8. Stable concomitant medications for depression, post-traumatic stress disorder, psychotic disorders, and bipolar spectrum disorders if one of the following: SSRI, SNRI, bupropion, MAOI, trazodone, Tricyclic, typical and atypical antipsychotics, lithium, antihistamine, alpha-adrenergic agent, nicotine replacement. 9. Stable concomitant medications: propranolol, prazosin, and clonidine if used for psychiatric reasons, and not to control hypertension at the Baseline Visit and unchanged on Study Day 1. 10. Provide informed consent. 11. Understand and follow Lifestyle Considerations per protocol. Exclusion Criteria: 1. Clinically at risk or unstable due to: 1. Active psychosis or mania that is impairing insight, decision-making, perception, or ability to provide informed consent as assessed by the PI or designee during the Screening or Baseline Visits, discussion with the outpatient treatment provider, or at Study Day 1. 2. Active suicidal ideation or intent as assessed by the PI or designee during the Baseline Visit interview or the C-SSRS on Study Day 1. 3. Chronic benzodiazepine use, or at significant risk for, or in a state of benzodiazepine withdrawal at the Screening or Baseline Visits, Study Day 1, or in discussion with the outpatient treatment provider. 4. Alcohol Use Disorder as assessed by the PI or designee with \> 14 drinks / week (average of \> 2 / day) at the Screening or Baseline Visits or Study Day 1 or in discussion with the outpatient treatment provider. 5. Seizure disorder; use of anti-convulsant for bipolar disorder, seizure, or chronic pain (including topiramate, gabapentin, carbamazepine, valproic acid) at the Screening or Baseline Visits or Study Day 1. 6. Cardiac abnormalities including arrythmia, conduction abnormality or baseline QTC prolongation (QTcF \> 450 males; 470 females); pacemaker, history of myocardial infarction at the Baseline Visit. 7. Hypertension, diabetes mellitus, cancer, liver, and/or kidney disease and associated medications at the Screening or Baseline Visits or at Study Day 1. 2. Abnormal safety laboratory results. 3. ALT or AST \> 3xs upper limit of normal at Baseline or Study Day 1. 4. Undiagnosed hypertension defined as: 1. Baseline Visit: BP \> 160 / 100 mmHg or heart rate \> 120 bpm 2. Study Day 1: BP ≥ 180 / 120 mmHg or heart rate ≥ 140 bpm that continues after 10 minutes of rest. 5. Temperature \> 38.1°C at the Baseline Visit. Temperature \> 38.9°C at the Study Day 1. 6. Medications that stimulate the dopamine system pre- or post-synaptically, including L-Dopa, lisdexamfetamine, modafinil, gabapentin, phenobarbital, etc.) at the Screening or Baseline Visits or Study Day 1. 7. Medications for addiction, ADHD, insomnia, or bipolar spectrum disorders involving dopamine system stimulants, benzodiazepines, barbiturates, or mood stabilizers active via GABA or glutamate receptor system (e.g. valproic acid, lamotrigine, carbamazepine, acamprosate, disulfiram) at the Screening or Baseline Visits or Study Day 1. 8. Use of naltrexone or acamprosate (active at opioid or glutamatergic receptors) at the Screening or Baseline Visits or Study Day 1. 9. Significant, active infection (e.g., positive for syphilis, tuberculosis, COVID-19, HBV) at the Baseline Visit. 10. Symptomatic HIV or HCV (detectable viral load) at the Baseline Visit. 11. Pregnancy or breastfeeding at the Screening or Baseline Visits or Study Day 1. 12. Poor venous access at the Baseline Visit or Study Day 1. 13. Participation in a research study involving another investigational drug in the last 3 months at the Screening Visit.
Where this trial is running
Indianapolis, Indiana
- Indiana University School of Medicine — Indianapolis, Indiana, United States (Recruiting)
Study contacts
- Study coordinator: Christopher Toombs
- Email: ctoombs@proniras.com
- Phone: 206-957-7321
How to participate
- Review the eligibility criteria above with your treating physician.
- Visit the official trial page on ClinicalTrials.gov for the most current contact information and recruitment status.
- Contact the listed study coordinator or principal investigator to request pre-screening. Pre-screening is free and never obligates you to enroll.