Nitrous Oxide as a Putative Novel Dual-Mechanism Treatment for Bipolar Disorder

Phase 2

Terminated

• Conditions: Bipolar Disorder
• Interventions: Drug: Nitrous Oxide; Drug: Midazolam

• Registration Number: NCT02351869
• Lead Sponsor: Sunnybrook Health Sciences Centre

Brief Summary

This study is a 7-day randomized, double-blind proof-of-concept pilot study of nitrous oxide vs. midazolam in 40 adults (20-60 years) with bipolar disorder (BD) (type I or II). Ongoing pharmacological and psychosocial treatments may continue, provided that they have not been initiated or significantly modified in the preceding 2 weeks. Participants' current treatment as prescribed by clinical psychiatrists will not be modified or interfered in this study. The study involves 3 visits. During study visit 1, participants will complete screening to ensure study eligibility. This will be done using interview measures. During study visit 2, participants will complete anthropomorphic measurements, measurement of endothelial function, screening blood work, ECGs, and an anaesthesia screener. During study visit 3, participants will receive the treatment (nitrous oxide or midazolam), complete an MRI scan, and complete interview measures and self-reports. There will be anthropomorphic measurements taken as well. The participant will be required to complete phone interviews and self-reports over the subsequent 7 days. There are 4 main predictions: 1. Nitrous oxide will significantly reduce depression symptoms vs. midazolam. 2. Nitrous oxide will significantly increase frontal cortical perfusion vs. midazolam. 3. Lower perfusion in frontal cortical regions at baseline will be associated with greater improvement in depression symptoms following nitrous oxide treatment. 4. Poorer endothelial function will be associated with greater improvement in depression symptoms following nitrous oxide treatment.

Detailed Description

Not available

Study Timeline

• Study First Submitted: 2014-12-02
• Study First Submitted QC: 2015-01-29
• Study First Posted: 2015-01-30
• Study Start: 2015-08
• Primary Completion: 2020-02-01
• Study Completion: 2020-06-07
• Status Verified: 2023-04
• Last Update Submitted: 2023-04-04
• Last Update Posted: 2023-04-06

Recruitment & Eligibility

• Status: TERMINATED
• Sex: All
• Target Recruitment: 25

Inclusion Criteria

English-speaking; age 20-60 years; BD-I or BD-II, current major depressive episode ≥4 weeks duration; MADRS≥22; taking ≥1 mood stabilizing medication/s (i.e. antimanic anticonvulsant, antipsychotic, and/or lithium).

Exclusion Criteria

New medications or changes in dosing, or ECT or TMS, in the preceding 2 weeks; MADRS item 10, > 4; YMRS≥12; acute significant suicidality; psychosis; substance abuse (past 3 months); active major medical conditions (hepatic, renal, respiratory, or cardio/cerebrovascular disease; diabetes; esophageal reflux; sleep apnea); B12 deficiency/disorders; pregnant; MRI contraindications; history of adverse anaesthetic reactions; anaesthesia class >2; scuba diving in preceding week.

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Nitrous oxide	Nitrous Oxide	N2O-condition participants will inhale an initial mixture of 10% N2O in oxygen (O2) for 5 minutes, followed by 25% N2O in O2 for 20 minutes. N2O-condition participants will also receive 5ml intravenous saline concomitantly with 10% N2O, and again with 25% N2O.
Midazolam	Midazolam	Inhaled room air plus intravenous midazolam bolus (total 2mg). Midazolam-condition participants will receive intravenous infusions of 0.5mg midazolam in 5ml saline (start of 1st inhalation epoch), followed by 1.5mg midazolam in 5ml saline (start of 2nd inhalation epoch).

Primary Outcome Measures

Name	Time	Method
Change in Montgomery-Asberg Depression Scale (MADRS) score	Assessed at baseline, an average of 3 days later, again at up to 5 days after baseline on the day of drug administration, and participants will be followed for 7 days after the drug administration	Measures mood symptom severity, used to select patients and assess treatment efficacy. Although other time-points will be examined, 24h was selected as the primary outcome to minimize the impact of acute sedation and psychoactive effects.

Secondary Outcome Measures

Name	Time	Method
Young Mania Rating Scale (YMRS)	Assessed at baseline, an average of 3 days later, again at up to 5 days after baseline on the day of drug administration, and participants will be followed for 7 days after the drug administration	Measures symptom severity
Blood Pressure	Measured an average of 3 days post-baseline and again approximately every hour on the drug administration day
Visual Analogue Scale	Assessed on the drug administration day and followed for 7 days post-drug administration
Height	Assessed an average of 3 days after baseline
Biomarkers (B12 and nitric oxide (NO))	Assessed an average of 3 days after baseline	B12 and nitric oxide (NO) will be examined as predictors of response owing to known associations with the mechanism of action of N2O.
The Clinician Administered Dissociative States Scale (CADSS)	Assessed on the drug administration day and followed for 7 days post-drug administration
General Information Sheet (Demographics)	Collected at baseline	Demographics
Hamilton Anxiety Rating Scale (HAM-A)	Assessed on the drug administration day and followed for 7 days post-drug administration	Interview measure used to assess anxiety severity
Hamilton Depression Rating Scale (HDRS)	Assessed on the drug administration day and followed for 7 days post-drug administration	Interview measure used to assess mood severity
Patient Rated Inventory of Side Effects	Assessed on the drug administration day and followed for 7 days post-drug administration	Self-report used to assess side effects
CANTAB Medication Listing	Assessed an average of 3 days after baseline	Used to collect medications taken the day before and on the day of blood work
Structured Clinical Interview for DSM Disorders	Assessed at baseline	Interview measure used to assess DSM disorders
Frontal Perfusion assessed using an MRI scan	Assessed approximately 5 days after baseline and post-drug administration	Will be assessed using an MRI scan.
Heart Rate	Measured an average of 3 days post-baseline and again approximately every hour on the drug administration day
Brief Psychiatric Rating Scale	Assessed on the drug administration day and followed for 7 days post-drug administration
Weight	Assessed an average of 3 days after baseline
Beck Depression Inventory (BDI-II)	Assessed on the drug administration day and followed for 7 days post-drug administration	Self-report measure of mood severity
Endothelial Function assessed via RH-PAT using the EndoPAT.	Assessed an average of 3 days after baseline and lasts approximately 30 minutes	Will be assessed via RH-PAT using the EndoPAT.

Trial Locations

Locations (1)

Sunnybrook Health Sciences Centre; 🇨🇦 Toronto, Ontario, Canada