Mirtazapine and Methamphetamine Drug-drug Interaction Study

Last updated: September 25, 2024
Sponsor: San Francisco Department of Public Health
Overall Status: Completed

Phase

1

Condition

Stimulant Use Disorder

Cardiovascular Abnormalities

Treatment

Mirtazapine

Methamphetamine

Clinical Study ID

NCT04614584
20-30109
  • Ages > 18
  • All Genders
  • Accepts Healthy Volunteers

Study Summary

This is a drug-drug interaction (DDI) study of mirtazapine for methamphetamine (MA) use disorder (MUD) to ensure the safety of this medication in the presence of a relevant dose of MA for people actively-using MA.

Aim 1: To determine if mirtazapine alters the cardiovascular response to IV MA.

Aim 2: To determine if the pharmacokinetics of IV MA are altered by mirtazapine administration.

Aim 3: To evaluate the above aims in the setting of concomitant administration of methadone.

This study involves two simultaneous within-subject drug-drug interaction studies, each comprised of 12 participants. A total of 24 subjects will be enrolled who have methamphetamine use disorder who will be classified into 2 groups: (Group 1: no opioids; Group 2: opioid use disorder on methadone maintenance). Subjects will be randomized to the order of mirtazapine and placebo (i.e. one-half will receive mirtazapine first, then placebo; one-half will receive placebo first, then mirtazapine).

Eligibility Criteria

Inclusion

Inclusion Criteria:

  1. English-speaking;

  2. age 18-55 years inclusive;

  3. meet DSM-V criteria for MA use disorder, as diagnosed via SCID;

  4. provide MA-positive urine during screening;

  5. have a resting heart rate of 50-90

  6. have a systolic blood pressure ≤ of 100-150 mm Hg, and diastolic blood pressure of 45-90 Hg within two days prior to admission;

  7. have a baseline EKG that demonstrates normal sinus rhythm, QTc < 440 msec in men orQTc < 450 msec in women;

  8. have acceptable safety lab data, ALT / AST<3x upper limit nL; est GFR >50;

  9. if female (except females of non-childbearing potential-e.g., at least 1 yearpost-menopausal or surgically sterile), not pregnant confirmed by negative pregnancytest nor lactating and willing to use a medically approved method of birth controlto prevent pregnancy during the trial and for 7 days after the last dose of studymedication.

  1. For those who also use opioids and are on methadone maintenance treatment (Group 2),urine positive for methadone and negative for buprenorphine on admission.

Exclusion

Exclusion Criteria:

  1. Have current cocaine, cannabis, or alcohol use disorder by DSM-V SCID;

  2. current or past history of seizure disorder;

  3. current ongoing treatment with psychotropic medications (e.g. antidepressants,antipsychotics, antiepileptics, sedative/hypnotics, narcotic analgesics);

  4. urine positive for MA and other unplanned drugs on the day of admission andbreathalyzer results negative for alcohol;

  5. any prior adverse reaction to MA; including chest pain or epileptic seizure;

  6. major psychiatric disorder not due to substance abuse (e.g., schizophrenia, bipolarillness but excepting stable major depressive disorder, generalized anxietydisorder, etc.) as assessed by the SCID;

  7. have a current neurological disorder (e.g., organic brain disease, dementia) ormedical condition which would make study compliance difficult or compromise informedconsent;

  8. history of suicide attempt(s) in the past 90 days or current suicidal intent or planby SCID;

  9. evidence of untreated or unstable serious medical illness including: neuroendocrine,autoimmune, renal, hepatic, or active infectious disease including activetuberculosis infection;

  10. seeking treatment for MA problems at the time of the study;

  11. any serious medical or psychiatric AE after test infusion of MA 30mg IV (e.g.sustained SBP>200 or DBP>100; sustained pulse >(220-0.85xAge).

  12. any other circumstances that, in the opinion of the investigators, would compromiseparticipant safety and/or successful completion of the trial.

Study Design

Total Participants: 15
Treatment Group(s): 2
Primary Treatment: Mirtazapine
Phase: 1
Study Start date:
May 03, 2021
Estimated Completion Date:
May 31, 2024

Study Description

This is a drug-drug interaction (DDI) study of mirtazapine for methamphetamine (MA) use disorder (MUD) to ensure the safety of this medication in the presence of a relevant dose of MA for people actively-using MA. MA is a widely used psychostimulant associated with substantial morbidity and mortality. MA is more prevalent than many other drugs, including opioids, with 37 million users of MA and amphetamine worldwide and 1.4 million past-year users in the U.S. alone in 2016. The number of MA poisoning deaths has steadily risen in recent years, from >3,700 in 2014 to 10,333 in 2017. Importantly, MA has been recognized as contributing substantially to the U.S. opioid crisis, with about half of MA poisoning deaths also caused by opioids. In the U.S., the annual economic cost of MA use is estimated to be $23.4 billion and use is strongly associated with HIV transmission.

There are no FDA-approved pharmacologic treatments for MUD, a major gap in addiction medicine, especially because behavioral interventions alone have limited efficacy and would likely benefit from adjunctive pharmacologic therapy. Investigators' prior clinical trials included a Phase IIa trial (N=60) and a replication Phase IIb trial (N=120) demonstrating that mirtazapine (an adrenergic, serotoninergic, and dopaminergic generic medication currently approved to treat depression) 30mg orally once daily reduced MA use among MA-dependent men who have sex with men (MSM) and transgender women. Investigators were directed to conduct a DDI study to ensure the safety of mirtazapine with MA. This research is particularly relevant given the overlap of MA use disorder and opioid use disorder (OUD), which could raise additional safety concerns.

The primary objectives of this study are as follows:

  1. To determine if mirtazapine 30mg daily alters the cardiovascular response to IV MA. The interaction of active medication (compared with placebo) with relevant doses of MA (30 mg) on cardiovascular (heart rate, blood pressure, QTc interval) parameters and adverse events, including serotonergic signs, will be assessed to gather safety information in the Phase I human laboratory.

  2. To determine if mirtazapine alters the pharmacokinetics of IV MA. Pharmacokinetic parameters for MA and its major metabolites will be assessed over 48 hours under steady state mirtazapine (30 mg) or placebo, and relevant IV MA challenge (30 mg).

  3. To evaluate the above aims in the setting of concomitant steady-state administration of morphine or methadone.

Design This study involves two simultaneous within-subject drug-drug interaction studies, each comprised of 12 participants. A total of 24 subjects will be enrolled who have MA use disorder who will be classified into 2 groups: (Group 1: no opioids; Group 2: opioid use disorder on methadone maintenance). Subjects will be randomized to the order of mirtazapine and placebo (i.e. one-half will receive mirtazapine first, then placebo; one-half will receive placebo first, then mirtazapine).

Procedures Screening assessments will be completed across two-to-four visits over 2 weeks. All screening assessments should be completed within 14 days after labs are drawn.

All subjects will complete the following study visits: screening 1 and 2, enrollment/admission to inpatient stay, 14-day inpatient stay, 14-day post-discharge follow-up visit.

After consent is obtained, eligibility will be determined over the following screening visits, including medical history and physical examination (including weight and height), review of systems, vital signs, concomitant medications, EKG, breathalyzer, labwork, SCID. Additional assessments will include the CDS-12, PSQI, TLFB for substance use, delayed discounting, BIS-11, Stroop Test, CUDIT-r, COWS, ACSA, BDI-II.

On the day of enrollment, study staff will confirm eligibility and transport patient to hospital for admission. Participant will receive a test infusion of MA 30mg IV. If participant tolerates test infusion within defined parameters, participant will be formally enrolled and randomized. First dose of study drug will be administered the evening of admission. On the fifth hospital day, participant will undergo MA challenge (single-blind placebo and 30mg IV for subjective, cardiovascular, and PK assessments). PK draws will continue for 48 hours after infusion.

Participant will begin the opposite condition on day 8 and complete the MA infusion procedures on day 12. After completion of PK studies on day 14, participant will be discharged.

A post-discharge safety check will be completed 10 days after discharge (+/- 7 days).

Connect with a study center

  • UCLA Medical Center

    Los Angeles, California 90095
    United States

    Site Not Available

  • San Francisco Department of Public Health

    San Francisco, California 94102
    United States

    Site Not Available

  • Substance Use Research Unit

    San Francisco, California 94102
    United States

    Site Not Available

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