- ICH GCP
- US Clinical Trials Registry
- Clinical Trial NCT03096353
Sensory and Opioid Mechanisms of Affective Touch
Background:
Medicines called opioids are used to treat pain. The body also produces opioids. These are called endorphins. Researchers want to learn more about how these natural opioids work. This might lead to new therapies for conditions like depression, anxiety, and chronic pain.
Objective:
To determine how opioids affect how pleasant or unpleasant it feels when the skin is touched, compressed, or heated.
Eligibility:
Healthy right-handed adults ages 18-50.
Design:
Participants will be screened under another protocol.
Participants will have 2 study visits with the same procedures, at least 1 day apart. Each visit will last 3-4 hours.
Participants will wear shorts or change into scrubs so researchers can test on their legs.
Participants will answer questions and have urine tests.
Participants will have a brain magnetic resonance imaging (MRI) scan. The scanner is a metal cylinder in a strong magnetic field. Participants will lie on a table that slides in and out of the cylinder. A device called a coil will be placed over the head.
During MRI, participants will have sensory testing. They will get several types of touch to the calf of the leg. These include gentle brushing of the skin, gentle compression of the calf with an inflation sleeve, and heat stimuli.
Participants will have an intravenous line placed each day. They will get naloxone 1 day and saline the other day. Participants will not be told which they get. Naloxone is a drug that blocks opioid receptors.
The MRI and sensory testing will then be repeated.
After each stimuli block, participants will rate the sensations as well as their mood and calmness/anxiety.
Study Overview
Detailed Description
Objective: Our recent pilot study found evidence suggesting that blocking endogenous opioid release increases the pleasantness associated with having the skin stroked. Deep pressure touch (observed in hugs and massage) also typically conveys a sense of pleasantness. This increased pleasantness contrasts with evidence that blocking endogenous opioid release increases pain. The current study will examine the role of endogenous opioids in the pleasantness of light skin stroking and deep pressure touch, and contrast it with their role in the unpleasantness of a painful heat stimulus. Further, it will examine the neural basis of observed perceptual changes, using fMRI. This study constitutes the first study of the K99 phase of a K99/R00 grant application recently submitted to National Center for Complementary and Integrative Health (NCCIH) by Dr. Laura Case.
Study Population: 30 healthy participants will be enrolled in the study.
Design: Participants will receive intravenous saline or intravenous naloxone on separate days to investigate the effect of mu-opioid antagonism on the intensity and pleasantness of superficial and deep affective touch and the intensity and unpleasantness of cutaneous heat pain. Using a double-blind cross-over design, functional Magnetic Resonance Imaging (fMRI) will be conducted during sensory testing before and after the infusion of each drug to examine the neural mediation of opioid effects on touch perception. Ratings of mood, anxiety, pain intensity, pleasantness/unpleasantness, wanting and liking will also be collected throughout the study session.
Outcome measures: We will compare subjective ratings (mood, calmness, anxiety, pleasantness, wanting, liking, pain intensity and unpleasantness) during naloxone and saline to: 1) Determine whether naloxone increases the pleasantness and/or intensity of affective touch (light brush and deep compression); 2) Determine whether naloxone increases the unpleasantness and/or intensity of cutaneous heat pain; 3) Determine the role of mood or anxiety changes in mediating the effect of endogenous opioids on these perceptual measures; 3) Determine changes in the brain activation related to these effects.
Study Type
Enrollment (Actual)
Phase
- Early Phase 1
Contacts and Locations
Study Locations
-
-
Maryland
-
Bethesda, Maryland, United States, 20892
- National Institutes of Health Clinical Center
-
-
Participation Criteria
Eligibility Criteria
Ages Eligible for Study
Accepts Healthy Volunteers
Genders Eligible for Study
Description
-INCLUSION CRITERIA:
All subjects must be:
- Between 18 and 50 years old.
- Right-handed (on Edinburgh Handedness Inventory).
- Fluent in English.
- Able to provide written informed consent.
EXCLUSION CRITERIA:
Overall exclusion criteria for the study:
- Unable to comply with study procedures (or does not rate stimuli as tolerable) or unable to schedule visits promptly (including inability to schedule the second session within approximately 14 days of the first session)
- Pregnancy or breastfeeding.
- Use of recreational drugs in the past month (e.g., marijuana, methylenedioxymethamphetamine (MDMA, 'ecstasy' or 'Molly'), Lysergic acid diethylamide (LSD), cocaine, methamphetamine, heroin, prescription and/or opioids).
- Congenital lower limb deficiency or amputation.
- Peripheral neuropathy, dermatological condition such as scars or burns, or has had a tattoo in the testing region within the previous four weeks that might influence cutaneous sensibility.
- Women who consume more than 7 alcoholic beverages per week, and men who consume more than 14 drinks per week.
- Current chronic pain condition or has had chronic pain in the past year (painful condition lasting more than six months), including ongoing treatment with medications for neuropathic pain (e.g. gabapentin, tricyclic antidepressants, pregabalin, tramadol)
- Major medical condition, such as kidney, liver, cardiovascular (including blood clots, hypertension, preexisting cardiac arrhythmia), autonomic, pulmonary, or neurological problems (e.g., seizure disorder ) or a chronic systemic disease (e.g., diabetes).
- Current diagnosis or pharmacological treatment of psychiatric disorders such as major depression, major anxiety-related problems, post-traumatic stress syndrome, bipolar disorder, psychosis, attention-deficit/hyperactivity disorder or current or lifetime alcohol or substance abuse disorders (as identified in study #16-AT-0077)
- Participant has metal in his/her body which would make having an MRI scan unsafe, such as pacemakers, medication pumps, aneurysm clips, metallic prostheses (including metal pins and rods, heart valves or cochlear implants), shrapnel fragments, permanent eye liner or small metal fragments in the eye that welders and other metal workers may have.
- Participant is uncomfortable in small closed spaces (has claustrophobia) so that he/she would feel uncomfortable in the MRI machine or cannot lie comfortably flat on his/her back for up to 75 minutes in the MRI scanner.
- Participants weighs more than 550 lbs.
- Participant has taken any pain medication other than an over-the-counter NSAIDs or acetaminophen within the last month or for more than one month on a continual basis within last six months.
- Previous participation in 13-AT-0143 (related study).
- NIH employees who are subordinates, relatives, or co-workers of the investigators, or NCCIH Division of Intramural Research (DIR) employees.
- Participants using medications that play into opioid pathways (e.g. loperamide or dextromethorphan), that could potentially interact with naloxone (naltrexone, methylnaltrexone, droperidol, fenfluramine and clonidine)
- Participant using any herbal supplements (such as yohimbine) due to risk of unknown dangerous interaction as there is no data for herbal preparations and naloxone.
- Participant has allergies to naloxone or similar drugs.
EXCLUSION CRITERIA FOR INIDIVIDUAL STUDY SESSION:
- Has consumed alcohol within 24 hours, shows signs of alcohol withdrawal syndrome, or has behavioral signs of intoxication will be excluded immediately and not have the possibility to reschedule their session.
Used topical pain-relieving creams in the testing area (e.g. methylsalicylate, capsaicin) within 24 hours of testing or used non-steroidal anti-inflammatory drugs (NSAIDS, e.g. aspirin, ibuprofen), acetaminophen, or naproxen within 3 days of testing*.
- To be determined during the pre-session screening. Participants who cannot refrain from these activities may have their session rescheduled up to two times. If the participant is found non-compliant during the second rescheduled appointment, he or she will be excluded from the study.
Study Plan
How is the study designed?
Design Details
- Primary Purpose: Basic Science
- Allocation: Non-Randomized
- Interventional Model: Crossover Assignment
- Masking: Quadruple
Arms and Interventions
Participant Group / Arm |
Intervention / Treatment |
---|---|
Experimental: Naloxone, then Placebo
Day one - During MRI session participant underwent sensory stimulus testing followed by bolus and infusion doses of naloxone (0.05 mg/kg bodyweight). When infusion levels reached stability, sensory testing was performed again. Day two - During MRI session participant underwent sensory stimulus testing followed by bolus and infusion doses of normal saline. When infusion levels reached stability, sensory testing was performed again. |
saline
We will be using naloxone at normal clinical doses as the study drug.
Naloxone is an opiate antagonist and has been used since the 1960 s to reverse the effects of opiate overdoses.
|
Experimental: Placebo, then Naloxone
Day one - During MRI session participant underwent sensory stimulus testing followed by bolus and infusion doses of normal saline. When infusion levels reached stability, sensory testing was performed again. Day two - During MRI session participant underwent sensory stimulus testing followed by bolus and infusion doses of naloxone (0.05 mg/kg bodyweight). When infusion levels reached stability, sensory testing was performed again. |
saline
We will be using naloxone at normal clinical doses as the study drug.
Naloxone is an opiate antagonist and has been used since the 1960 s to reverse the effects of opiate overdoses.
|
What is the study measuring?
Primary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Change in Pleasantness of Skin Brushing From Before to After Infusion
Time Frame: One day, within a 2 hour session
|
Measurement of brushing pleasantness using a visual analogue scale.
Sensory hedonics (unpleasantness vs. pleasantness) was assessed on a scale ranging from extremely unpleasant (-100) to neutral (0), to extremely pleasant (100).
|
One day, within a 2 hour session
|
Secondary Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Changes in Pleasantness of Deep Skin Pressure From Before to After Infusion
Time Frame: One day, within a 2 hour session
|
Measurement of pressure pleasantness/unpleasantness using a visual analogue scale.
Sensory hedonics (unpleasantness vs. pleasantness) was assessed on a scale ranging from extremely unpleasant (-100) to neutral (0), to extremely pleasant (100).
|
One day, within a 2 hour session
|
Change in Unpleasantness of Cutaneous Heat Pain From Before to After Infusion
Time Frame: One day, within a 2 hour session
|
Measurement of heat pleasantness/unpleasantness using a visual analogue scale.
Sensory hedonics (unpleasantness vs. pleasantness) was assessed on a scale ranging from extremely unpleasant (-100) to neutral (0), to extremely pleasant (100).
|
One day, within a 2 hour session
|
Changes in Intensity of Skin Brushing From Before to After Infusion
Time Frame: One day, within a 2 hour session
|
Measurement of brushing intensity using a visual analogue scale.
Intensity was assessed on a scale ranging from no sensation (-100) to pain threshold (0), to intolerable pain (100).
|
One day, within a 2 hour session
|
Changes in Intensity of Deep Skin Pressure From Before to After Infusion
Time Frame: One day, within a 2 hour session
|
Measurement of pressure intensity using a visual analogue scale.
Intensity was assessed on a scale ranging from no sensation (-100) to pain threshold (0), to intolerable pain (100).
|
One day, within a 2 hour session
|
Changes in Intensity of Cutaneous Heat Pain From Before to After Infusion
Time Frame: One day, within a 2 hour session
|
Measurement of heat intensity using a visual analogue scale.
Intensity was assessed on a scale ranging from no sensation (-100) to pain threshold (0), to intolerable pain (100).
|
One day, within a 2 hour session
|
Other Outcome Measures
Outcome Measure |
Measure Description |
Time Frame |
---|---|---|
Activation in Somatosensory Cortex (S2) Brain Area of Interest (ROI) During Brushing
Time Frame: One day, within a 2 hour session
|
Functional MRI Blood-oxygen-level-dependent (BOLD) activation in secondary somatosensory cortex (S2) during brushing.
BOLD signal is typically expressed as arbitrary units (AU's) measured from "0 to 100% change".
0 being no change and 100% maximum change
|
One day, within a 2 hour session
|
Activation in Somatosensory Cortex (S2) Brain Area of Interest (ROI) During Pressure
Time Frame: One day, within a 2 hour session
|
Functional MRI Blood-oxygen-level-dependent (BOLD) activation in secondary somatosensory cortex (S2) during pressure.
BOLD signal is typically expressed as arbitrary units (AU's) measured from "0 to 100% change".
0 being no change and 100% maximum change
|
One day, within a 2 hour session
|
Changes in Mood During Skin Brushing From Before to After Infusion
Time Frame: One day, within a 2 hour session
|
Mood during brushing was assessed using a visual analogue scale ranging from extremely bad mood (-100) to neutral mood (0), to extremely good mood (100).
|
One day, within a 2 hour session
|
Changes in Mood During Skin Pressure From Before to After Infusion
Time Frame: One day, within a 2 hour session
|
Mood during skin pressure was assessed using a visual analogue scale ranging from extremely bad mood (-100) to neutral mood (0), to extremely good mood (100).
|
One day, within a 2 hour session
|
Changes in Mood During Cutaneous Heat From Before to After Infusion
Time Frame: One day, within a 2 hour session
|
Mood during heat was assessed using a visual analogue scale ranging from extremely bad mood (-100) to neutral mood (0), to extremely good mood (100).
|
One day, within a 2 hour session
|
Changes in Anxiety During Skin Brushing From Before to After Infusion
Time Frame: One day, within a 2 hour session
|
Anxiety during brushing was assessed using a visual analog scale ranging from extreme anxiety (-100) to neutral (0) to extreme calm (100).
|
One day, within a 2 hour session
|
Changes in Anxiety During Deep Skin Pressure From Before to After Infusion
Time Frame: One day, within a 2 hour session
|
Anxiety during pressure was assessed using a visual analog scale ranging from extreme anxiety (-100) to neutral (0) to extreme calm (100).
|
One day, within a 2 hour session
|
Changes in Anxiety During Cutaneous Heat From Before to After Infusion
Time Frame: One day, within a 2-hour session
|
Anxiety during heat was assessed using a visual analog scale ranging from extreme anxiety (-100) to neutral (0) to extreme calm (100).
|
One day, within a 2-hour session
|
Collaborators and Investigators
Investigators
- Principal Investigator: Catherine Bushnell, Ph.D., National Center for Complementary and Integrative Health (NCCIH)
Publications and helpful links
Helpful Links
Study record dates
Study Major Dates
Study Start (Actual)
Primary Completion (Actual)
Study Completion (Actual)
Study Registration Dates
First Submitted
First Submitted That Met QC Criteria
First Posted (Actual)
Study Record Updates
Last Update Posted (Actual)
Last Update Submitted That Met QC Criteria
Last Verified
More Information
Terms related to this study
Additional Relevant MeSH Terms
Other Study ID Numbers
- 170075
- 17-AT-0075
Drug and device information, study documents
Studies a U.S. FDA-regulated drug product
Studies a U.S. FDA-regulated device product
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