Clinical Trial Details
— Status: Recruiting
Administrative data
| NCT number |
NCT05751096 |
| Other study ID # |
IRB-22-1597 |
| Secondary ID |
|
| Status |
Recruiting |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
July 15, 2023 |
| Est. completion date |
January 2025 |
Study information
| Verified date |
October 2023 |
| Source |
Carilion Clinic |
| Contact |
Jessica Florig, MPH |
| Phone |
540-526-2261 |
| Email |
jnw[@]vtc.vt.edu |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Study investigating the potential benefit for chronic pain patients (CRPS and FM) using
low-intensity focused ultrasound for neuromodulation.
Description:
Before coming up with a low-intensity focused ultrasound (LIFU) therapy for complex regional
pain syndrome (CRPS) and fibromyalgia (FM) by running a clinical trial, the investigators
must run a proof-of concept study to understand whether LIFU neuromodulation will elicit
behavior and physiological responses in both these populations. The first study will be to
run a counterbalanced within subject design, of active or inactive LIFU. The order of the
sham vs real LIFU will be randomized on separate visits. The primary objective is to test if
LIFU will reduce pain sensation and a secondary objective to test if LIFU will improve
clinical outcomes, including changes in skin temperature and swelling circumference (in
centimeters) of the target limb. The target limb is defined for CRPS as the injured extremity
(upper or lower limb) and for FM as the dominant upper extremity. These clinical outcomes are
common for both CRPS and FM population, along with pain, and these measurements are being
taken to see if LIFU will affect these clinical features. LIFU has been tested extensively on
healthy participants, demonstrating changes in brain activity without any damage.
An ultrasound transducer is the device used to apply LIFU, which will be fitted onto the
scalp using a real-time head tracking infrared camera. Brief low-intensity ultrasound pulses
will be delivered. Quantitative sensory testing (QST) will be utilized to cause a pain
response by placing a thermode on the skin of the hand, forearm, lower leg, or foot and the
temperature will be raised or lowered at a set rate. There will be four separate QST
protocols including thermal thresholding, conditioned pain modulation (CPM), temporal
summation of pain (TSP) and contact heat provoked potential (CHEP).
Thermal pain threshold testing will be established on the target limb to determine the
individualized baselines for additional testing protocols. The QST device will be set to a
baseline temperature of 32° C and increased at a rate of 1° C/sec. Once the participant feels
pain from the heat stimulus, a button that returns the temperature to baseline will be
pressed. This process will repeat 5 times and the average threshold will be calculated. CPM
involves the co-delivery of a conditioned stimulus and a test stimulus. For the conditioned
cold stimulus, the patients will submerge their opposite limb (of target limb) in a bucket of
ice water, and it will be followed by the test stimulus, a heat stimulus to the target limb.
The patients will then rate the perceived pain on a 10-point scale and the entire procedure
will be repeated 3 times before and after LIFU stimulation. For TSP, heat stimulation is
applied to the selected site. The baseline is set and is increased up to a destination
temperature determined by individuals threshold testing and then either remains constant or
pulses for up to 180 seconds. Subjects will rate the magnitude of perceived pain either
verbally or numerically using a 10-point scale and the procedure will be performed 3 times
before and after LIFU stimulation. For CHEP, the heat stimuli are given at random intervals
between 10-20 seconds on multiple varied locations on the target limb to avoid habituation
and heating. Patients will rate 40 stimuli on a perceived pain 10-point scale before and
after LIFU stimulation and brain responses recorded using electroencephalography (EEG).
Non-contact infrared thermometers will be used to take skin temperature of the target limb
and soft tape measures will be used to measure (in centimeters) the largest circumference
(region of inflammation for CRPS patients and variable for FM patients depending on which
muscle is larger) of the target limb.
A total of 15 CRPS patients and 12 FM patients will be enrolled in the study, with the
Carilion Clinic Pain Management physicians using the established Budapest Criteria to
diagnose CRPS type I and type II. The first session will involve obtaining MRI and CT
anatomical scans, needed to accurately target the area of interest (anterior insula) during
the QST sessions and ensure accurate application of the LIFU for each individual. Baseline
clinical measurements of the target limb will also be obtained. The next two sessions will be
randomly counterbalanced with LIFU or sham while obtaining QST and clinical measurements.
Blood pressure, respiratory rate, galvanic skin response, photoplethysmography, and two-lead
electrocardiogram will also be collected to monitor the patient's autonomic nervous system
changes as potential confounding factors as well as assessing for effects from the
ultrasound. Questionnaires will be administered via Redcap throughout each session to
document potential confounding factors such as depression, fear and anxiety while also
recording the patient's symptoms before and after LIFU application. Brief pain inventory
(BPI) will also be documented for the CRPS participants, measuring both the intensity of pain
and the interference of pain in the patient's life along with the revised fibromyalgia impact
questionnaire (FIQR) for the FM participants.
