SPIN-CWP: Sleep and Pain Intervention for Chronic Widespread Pain Pilot Study

Sponsor

University of Missouri-Columbia (Other)

Overall Status

Recruiting

CT.gov ID

NCT02688569

Collaborator

(none)

Enrollment

Location

Arms

Anticipated Duration (Months)

0.3

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

This randomized controlled clinical trial will examine the effects of Cognitive Behavioral Therapy (CBT-) in patients with comorbid chronic widespread pain (CWP) and insomnia.

Specific Aims:

To examine the clinical and health characteristics, including sleep, pain, fatigue, cognitive abilities, and cardiovascular health in patients with comorbid CWP and insomnia.
To examine changes in the primary clinical outcomes, including chronic pain, complaints of poor sleep, and fatigue compared to the waitlist control (WLC).
To examine changes in the secondary clinical outcomes, including mood, daytime functioning, cognitive functioning, and cardiovascular health compared WLC.
To examine the mechanistic variables, including arousal (heart rate variability, HRV), CS (thermal response) and neural plasticity (brain function and structure) - compared to WLC.

Condition or Disease	Intervention/Treatment	Phase
Chronic Widespread Pain Chronic Insomnia	Behavioral: Cognitive Behavioral Therapy for Chronic Widespread Pain	N/A

Detailed Description

This randomized controlled clinical trial will examine the effects of CBT in patients with chronic widespread pain and insomnia. Sample will include 20 patients ([18]-65 years) who satisfy criteria for chronic widespread pain and insomnia. Participants will be randomly assigned to CBT or waitlist control. All participants randomized to the cognitive-behavioral interventions will receive 4 treatment sessions (~50 minutes each). Baseline, posttreatment, [& 3-mo.] follow-up assessments will include measures of sleep, pain, thermal pain response, heart rate variability, brain structure and functions, affect, cognitive functioning, cardiovascular health, and substance use.

Study Design

Study Type:

Interventional

Anticipated Enrollment :

20 participants

Allocation:

Randomized

Intervention Model:

Parallel Assignment

Masking:

None (Open Label)

Primary Purpose:

Treatment

Official Title:

Sleep and Pain Intervention for Chronic Widespread Pain Pilot Study

Actual Study Start Date :

Oct 1, 2016

Anticipated Primary Completion Date :

Dec 1, 2022

Anticipated Study Completion Date :

Dec 1, 2022

Arms and Interventions

Arm	Intervention/Treatment
Experimental: CBT-CWP Participants in this condition will receive Cognitive Behavioral Therapy for Chronic Widespread Pain (CBT-CWP)	Behavioral: Cognitive Behavioral Therapy for Chronic Widespread Pain CBT-CWP in this study involves 4 sessions of one-hour non-drug behavioral intervention. Session 1 involves education about pain and insomnia and the relationship between the two. Participants will also learn sleep hygiene and stimulus control skills. Session 3 involves teaching participants skills to limit non-sleep time in bed and thus increase sleep efficiency. Participants will also learn the relationship between pain and activity. Session 4 involves teaching participants cognitive restructuring and mindfulness skills to manage maladaptive thoughts related to pain and insomnia. Participants will also review the skills they learned and discuss the maintenance of treatment gains. Other Names: CBT-CWP
No Intervention: Control Participants in the Control condition will not receive CBT-CWP. They will however, continue completing the weekly assessments.

Arm

Intervention/Treatment

Experimental: CBT-CWP

Participants in this condition will receive Cognitive Behavioral Therapy for Chronic Widespread Pain (CBT-CWP)

Behavioral: Cognitive Behavioral Therapy for Chronic Widespread Pain

CBT-CWP in this study involves 4 sessions of one-hour non-drug behavioral intervention. Session 1 involves education about pain and insomnia and the relationship between the two. Participants will also learn sleep hygiene and stimulus control skills. Session 3 involves teaching participants skills to limit non-sleep time in bed and thus increase sleep efficiency. Participants will also learn the relationship between pain and activity. Session 4 involves teaching participants cognitive restructuring and mindfulness skills to manage maladaptive thoughts related to pain and insomnia. Participants will also review the skills they learned and discuss the maintenance of treatment gains.

Other Names:

CBT-CWP

No Intervention: Control

Participants in the Control condition will not receive CBT-CWP. They will however, continue completing the weekly assessments.

Outcome Measures

Primary Outcome Measures

Change in self-reported ratings of Pain Sensitivity and Pain Unpleasantness on Daily Diaries [Participants will complete the pain ratings daily for 56 days from Baseline to Post-Treatment , and for 14 days in 3-month Follow-Up (Week 21-22)]
Participants will rate how much pain they experience and how unpleasant the pain is on a scale of 1 to 100 on the daily dairies. Analysis will involve examining the trend of changes in these ratings.
Change in pain severity assessed by the McGill Pain Questionnaire [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
The McGill Pain Questionnaire will be administered three times - baseline, post-treatment, and follow-up. Analysis will involve examining the trend of change in the scores in McGill Pain Questionnaire.
Change in pain-associated disability assessed by the Pain Disability Questionnaire [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
The Pain Disability Questionnaire will be administered three times - baseline, post-treatment, and follow-up. Analysis will involve examining the trend of change in the scores in Pain Disability Questionnaire.
Change in Self-Reported Bedtime, Wake time, Sleep Onset Latency, Wake After Sleep Onset, Sleep Quality on the Daily Diaries [Participants will complete the sleep questions daily for 56 days from Baseline to Post-Treatment , and for 14 days in 3-month Follow-Up (Week 21-22)]
Participants will answer the following questions on the daily diaries: I napped for ____________ minutes yesterday. I napped ______ times yesterday. I napped in the ___morning ___afternoon ____evening (check all that apply) I went to bed last night at ____________ AM/PM. It took me ____________ minutes to fall asleep. I woke up ____________ times last night. I was awake for ____________ minutes in the middle of the night. My final wake up time was ____________ AM/PM. I got out of bed at ____________ AM/PM. I would rate my quality of sleep last night as ____________. 1. very poor 2. poor 3. fair. 4 good 5. Excellent
Change in Bedtime, Wake time, Sleep Onset Latency, and Wake After Sleep Onset measured by Actigraphy [Daily from the start of the study to post-treatment (week1 to week8), two-week daily reports in 3-mo follow up (week21,week22)]
Actiwatch-L (ACT-L; Mini Mitter, Inc.) will be used to obtain a behavioral measure of sleep outcome. ACT-L is a wristwatch-like device that provides long-term monitoring of ambient light exposure and gross motor activity in human subjects. The Actiware-Sleep software provides behavioral estimates for several sleep variables: (1) sleep onset latency-interval between bedtime and sleep start; (2) total sleep time-sum of all sleep epochs within the sleep period; (3) sleep efficiency percentage- ratio of total sleep time to total time spent in bed × 100; and (4) total wake time-sum of all wake epochs within the sleep period.
Change in Insomnia Severity Index [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
The Insomnia Severity Index will be administered three times - baseline, post-treatment, and follow-up. Analysis will involve examining the trend of change in the Insomnia Severity Index.

Secondary Outcome Measures

Change in heart rate variability [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
Change in Body Mass Index [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
Change in Cognitive Functioning measured by the NIH toolbox Cognitive Domain [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
Day-to-day change in Cognitive Functioning measured by the Cognitive Diary [Participants will complete cognitive diary daily for 56 days from Baseline to Post-Treatment , and for 14 days in 3-month Follow-Up (Week 21-22)]
Change in daily substance use [Participants will report daily substance use for 56 days from Baseline to Post-Treatment , and for 14 days in 3-month Follow-Up (Week 21-22)]
Participants will answer these questions: Drug Used________________ Prescription Drug? Y/N If yes, used as directed? Y/N Amount taken______________ Time taken________________
Change in Thermal Pain Response [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
Participants will undergo quantitative sensory testing using a contact thermode applied to the volar surface of the forearm. The protocol that will assess both first pain (primarily A-delta function) and second pain (primarily C-fiber input). All thermal stimuli will be delivered using a computer-controlled Medoc Thermal Sensory Analyzer (TSA-2001, Ramat Yishai, Israel). Visual Analog Scale (VAS) ratings of 4 graded intensities (45, 47, 49, 51° C) of 5 second temperature stimuli will be obtained in the following fashion: Stimulus presentation will be timed such that no site is stimulated with less than a 3-minute interval to avoid sensitization of the site. Participants will rate 8 stimuli (2 at each intensity) using a VAS for pain intensity anchored at the right end by "the most intense pain imaginable." A second random sequence of 8 stimuli (2 at each intensity) will be rated by VAS for pain unpleasantness.
Change in food habits measured by 24-hour dietary recall [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
Change in waist-to-hip ratio [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
Change in blood pressure [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
Change in alcohol use frequency as measured by the Alcohol Use Questionnaire [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
Change in alcohol problems as measured by the Alcohol Use Disorders Identification Test [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
Change in grey matter volume as measured by Structural MRI [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
Change in cortical thickness as measured by Structural MRI [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]
Change in functional connectivity in response to thermal pain stimuli as measured by Functional MRI [Pre-treatment (week1 or 2), post-treatment (week7 or 8), follow-up (week 21 or 22)]

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years and Older

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Inclusion Criteria:

18+ years old
Be willing to be randomly assigned to either the treatment condition or the control condition
Be able to read and understand English
Have Chronic Widespread Pain (CWP) and Insomnia based on the criteria below:

o CWP:

Complaints of pain in upper, lower body, on both sides and the back that lasts for 3+ months.
Not explained by other illnesses except somatic disorders.

o Insomnia:

Insomnia complaints for 6+ months
Occur despite adequate opportunity and circumstances for sleep
Consist of 1 or more of the following: difficulty falling asleep, staying asleep, waking up too early, nonrestorative sleep
Daytime dysfunction (mood, cognitive, social, occupational) due to insomnia
Baseline diaries indicate >30 minutes of sleep latency or wake after sleep onset combined on 6+ nights.

Exclusion Criteria:

Be unable to provide informed consent
Be unwilling to undergo randomization
Be unable to complete forms and implement treatment due to cognitive impairment (Mini Mental State Examination <26)
Sleep disorder other than insomnia (i.e., sleep apnea [apnea/hypopnea index, AHI >15]; Periodic Limb Movement Disorder-PLMD [myoclonus arousals per hour >15])
bipolar or seizure disorder
other major psychopathology except depression or anxiety (e.g., suicidal ideation/intent, psychotic disorders)
severe untreated psychiatric comorbidity that renders randomization unethical,
psychotropic or other medications (e.g., beta-blockers) that alter pain or sleep
participation in any nonpharmacological treatment (including CBT) for pain, sleep, fatigue, or mood outside the current study,
internal metal objects or electrical devices
pregnancy

Contacts and Locations

Locations

	Site	City	State	Country	Postal Code
1	Department of Health Psychology, University of Missouri-Columbia	Columbia	Missouri	United States	65203

Sponsors and Collaborators

University of Missouri-Columbia

Investigators

Principal Investigator: Christina S McCrae, Ph.D., University of Missouri-Columbia

Study Documents (Full-Text)

None provided.

More Information

Publications

Responsible Party:

Christina McCrae, Professor and Chair, University of Missouri-Columbia

ClinicalTrials.gov Identifier:

NCT02688569

Other Study ID Numbers:

2004488HS

First Posted:

Feb 23, 2016

Last Update Posted:

May 25, 2022

Last Verified:

May 1, 2022

Individual Participant Data (IPD) Sharing Statement:

Plan to Share IPD:

Additional relevant MeSH terms:

Sleep Initiation and Maintenance Disorders

Chronic Pain

Study Results

No Results Posted as of May 25, 2022