Effects of Pharmacological Stress and rTMS on Executive Function in Opioid Use Disorder

Phase 2

Not yet recruiting

• Conditions: Opioid Use Disorder
• Interventions: Drug: Placebo; Device: Active rTMS; Drug: Yohimbine + Hydrocortisone; Device: Sham rTMS

• Registration Number: NCT04231708
• Lead Sponsor: Wayne State University

Brief Summary

This preliminary study is designed to evaluate mechanisms by which excitatory dorsolateral prefrontal cortex (dlPFC) repetitive transcranial magnetic stimulation (rTMS) (vs. sham) and pharmacological stress (vs. placebo) alter behavior in non-treatment seeking individuals with opioid use disorder (OUD). Specific Aims are to (1) Evaluate how stress impacts domains of behavior including (1a) executive function and (1b) opioid-seeking behavior; and (2) Determine whether rTMS stimulation attenuates (2a) executive dysfunction, (2b) stress-reactivity, and (2c) opioid-seeking in individuals with OUD not receiving treatment.

Detailed Description

This study will use a double-blind, 10Hz left dlPFC rTMS (vs. sham) and pharmacological stressor (\[yohimbine + hydrocortisone\] vs. placebo) within-subject, randomized crossover design. Each participant will complete 4 sessions (stressor vs. placebo, crossed with rTMS vs. sham), each separated by at least 1 week. Participants will complete these 4 (2x2 within subject) test conditions in randomized order: sham rTMS/placebo stress, sham rTMS/active stress, active rTMS/ placebo stress, and active rTMS/active stress.

The PI will perform randomization using a Latin Square and will assign participants to conditions and prepare medication (stressor or placebo) for each participant's sessions. The PI will keep others blinded and will not be involved in study assessments.

Study Timeline

• Study First Submitted: 2020-01-09
• Study First Submitted QC: 2020-01-13
• Study First Posted: 2020-01-18
• Status Verified: 2024-12
• Last Update Submitted: 2024-12-14
• Last Update Posted: 2024-12-17
• Study Start: 2025-06
• Primary Completion: 2027-10
• Study Completion: 2027-12

Recruitment & Eligibility

• Status: NOT_YET_RECRUITING
• Sex: All
• Target Recruitment: 20

Inclusion Criteria

• Meet DSM-5 criteria for OUD;
• Age 21-60 yr;
• Right handed;
• Males and non-pregnant/non-lactating females;
• cognitively intact (total IQ score >80 on Shipley Institute of Living Scale);
• Screening cardiovascular indices within ranges for safe use of the pharmacological stressor: resting HR 50-90 bpm, systolic BP 90-140 mmHg, and diastolic BP 50-90 mmHg;
• Use alcohol and/or marijuana <3 times/week; each "time" should consist of <1 marijuana "joint" equivalent and <3 alcoholic drinks.

Exclusion Criteria

• Under influence of any substance during session;
• Past 7-day use of illicit drugs other than opioids (except marijuana, which is legal in Michigan);
• Urinalysis positive for cocaine metabolites, benzodiazepines, barbiturates, amphetamines or pregnancy;
• Medical conditions prohibiting use of rTMS (e.g. seizure history; based on rTMS screening questionnaire);
• Lifetime diagnosis of: psychotic disorder, bipolar disorder, generalized anxiety disorder, or obsessive compulsive disorder; major depression in the past 5 years; or potentially antisocial personality disorder (if the clinical psychologist judges such behaviors to be potentially disruptive or unsafe in our lab);
• Past-year SUD other than OUD;
• Acute/unstable illness: conditions making it unsafe for participation (e.g. neurological, cardiovascular, pulmonary, or systemic diseases);
• Lactose intolerance (placebo dose);
• Any prohibited medications: medications that lower seizure threshold, psychiatric medications, prescription pain medications, or blood pressure medications;
• Chronic head or neck pain; and
• Past-month participation in a research study.

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: CROSSOVER

Arm && Interventions

Group	Intervention	Description
placebo stressor, sham rTMS	Placebo	Placebo stressor (lactose) + sham (inactive) rTMS over the left dlPFC
placebo stressor, sham rTMS	Sham rTMS	Placebo stressor (lactose) + sham (inactive) rTMS over the left dlPFC
placebo stressor, active rTMS	Active rTMS	Placebo stressor (lactose) + active 10Hz rTMS over the left dlPFC
placebo stressor, active rTMS	Placebo	Placebo stressor (lactose) + active 10Hz rTMS over the left dlPFC
active stressor, sham rTMS	Yohimbine + Hydrocortisone	Stressor (yohimbine 54mg + hydrocortisone 20mg) + sham (inactive) rTMS over the left dlPFC
active stressor, sham rTMS	Sham rTMS	Stressor (yohimbine 54mg + hydrocortisone 20mg) + sham (inactive) rTMS over the left dlPFC
active stressor, active rTMS	Yohimbine + Hydrocortisone	Stressor (yohimbine 54mg + hydrocortisone 20mg) + active 10Hz rTMS over the left dlPFC
active stressor, active rTMS	Active rTMS	Stressor (yohimbine 54mg + hydrocortisone 20mg) + active 10Hz rTMS over the left dlPFC

Primary Outcome Measures

Name	Time	Method
Color-Word Stroop Task	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	measures cognitive control in response to opioid-related words.
Digit Span Task	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	measures verbal working memory. Participants are asked to repeat strings of numbers of increasing length, both forward and backward.
Positive and Negative Affect Schedule	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	subjects rate their positive and negative affect
State-Trait Anxiety Inventory	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	subjects rate their level state anxiety
Diastolic blood pressure	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	millimeters mercury (mmHg)
Saliva cortisol level	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	measure of the activity of the HPA axis
Relative electroencephalogram (EEG) gamma power	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	Prefrontal gamma (25-100 Hz) EEG power, relative to slow-wave EEG power, is a stress biomarker
Drug/Money Choice Task	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	participants choose hypothetically between a constant amount of their preferred opioid ($10 unit dose) or money ($2)
Systolic blood pressure	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	millimeters mercury (mmHg)
Heart rate	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	beats per minute
Serum brain derived neurotrophic factor (BDNF) level	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	indirect measure of brain derived neurotrophic factor activation
Wisconsin Card Sorting Task	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	measures ability to shift set and assesses cognitive flexibility.
Saliva alpha-amylase level	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	indirect measure of adrenergic stimulation
Emotion Regulation Task	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	subjects rate the unpleasantness and arousal of different emotional pictures
Monetary Incentive Delay Task	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	Participants respond to a visual target that follows 2 different cues: incentive or non-incentive. No reward or punishment occurs on non-incentive trials. On incentive trials, participants must respond within a fixed amount of time. In the reward condition, responses within that time result in receiving the incentive , else nothing. In the punishment condition, the participant will lose money if they do not respond within the time limit
Delay Discounting Task	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	Participants perform a brief (\<1min) hypothetical version of the traditional monetary task with a 5-trial adjusting delay previously validated to rapidly assess discount rate
Serum prolactin level	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	indirect measure of dopamine stimulation

Secondary Outcome Measures

Name	Time	Method
Opioid craving	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	Desire for Drug Questionnaire total score; higher scores indicate greater craving
Opioid withdrawal symptoms	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	Opiate-32 questionnaire withdrawal symptom total score; higher scores indicate greater withdrawal severity
Opioid agonist symptoms	change from pre- to post-intervention in each of 4 sessions (through study completion, about 1 month total)	Opiate-32 questionnaire agonist symptom total score; higher scores indicate greater opioid symptom severity

Trial Locations

Locations (1)

Tolan Park Medical Building; 🇺🇸 Detroit, Michigan, United States