Contemplation-Based Intervention and Health Outcomes RCT in Lupus Patients

December 19, 2019 updated by: William Cunningham, University of Toronto

A Randomized Controlled Trial to Investigate a Contemplation-Based Intervention and Health Outcomes in Systemic Lupus Erythematosus Patients

The objective of this study is to test the efficacy of an innovative contemplative-based and caregiver-inclusive intervention can modify pathogenic processes in systemic lupus erythematosus (SLE) compared to a psychoeducation-based intervention. Contemplative techniques such as meditation, mindfulness and yoga may have an impact on the disease burden and may decrease psychological distress, increase self-regulation capabilities, and reduce pain. It is also well documented that social relationships moderate physical health. Incorporating patients' caregivers may strengthen their relationships and thereby improve their health and well-being. It is anticipated that the successful outcome of the mindfulness-based intervention described in this proposal will provide the basis for a new and effective contemplative-based and caregiver-inclusive therapy for SLE and other rheumatic diseases. Although we expect our mindfulness-based intervention to outperform our psychoeducation intervention, we note that the psychoeducation intervention is much closer to treatment as usual (especially insofar as many lupus patients are provided no psychosocial intervention whatever), and to that degree can reasonably be considered our best initial point of comparison. In practice, most patients would be provided medication and some basic information about living with the disease, as well as, perhaps, some additional guidance about coping with chronic stress and pain. We believe that our comparison condition goes beyond this to provide a bona fide intervention in itself.

Study Overview

Detailed Description

METHODS: A randomized controlled trial of 50 SLE patients in which subjects receive either a 6-week MBI treatment (n=25) or a 6-week psychoeducation treatment (n=25).

SCREENING: At Visit 1, participants who are deemed eligible for the study will be assigned to either a mindfulness-based intervention group or a psychoeducation intervention group. Participants will also complete the following questionnaires, which will also be administered throughout the intervention schedule:

  1. Adverse Childhood Experience (ACE)
  2. Adult Attachment Style Questionnaire (AAS; closeness subscale)
  3. Brief Health Mindset Scale (BHMS)
  4. Center for Epidemiological Studies Depression Scale Revised (CESD-R)
  5. Inclusion of Other Self (IOS)
  6. Interpersonal Reactivity Index (IRI; empathic concern and perspective-taking subscales)
  7. Interpersonal Regulation Questionnaire (IRQ)
  8. LupusPRO (patient only)
  9. MacArthur Scales of Subjective Social Status (Community and Socioeconomic Status)
  10. Caregiver Burden Questionnaire (support person only)
  11. Multidimensional Scale of Perceived Social Support (MSPSS)
  12. Pain Catastrophizing Scale (PCS)
  13. Ruminative Responses Scale (RRS; short form)
  14. Social Interaction Phobia Scale (SIPS)
  15. State Trait Anxiety Inventory (STAI-T, STAI-S)
  16. Ten Item Big Five Questionnaire
  17. Toronto Mindfulness Scale (TMS)
  18. Lupus Quality of Life
  19. CAM Health Belief Questionnaire

INTERVENTIONS: All participants will complete either a 6-week mindfulness-based intervention or a 6-week psychoeducation intervention. All sessions will be in-person in a group setting, and accompanied by homework. For both interventions, participants will practice what they learned on a daily basis as their homework. However, the mindfulness intervention may also have video/audio homework to complete. Sessions 1-5 will last approximately 2 hours each. The final (6th) session will be a retreat that will last approximately 4 hours. Questionnaire data will be collected throughout the intervention.

ASSESSMENTS: Assessment visits 1 and 9 will be performed by rheumatologists and include: complete history, physical examination, information about SLE drug treatment and laboratory examination. Lupus disease activity and damage will be measured by Systemic Lupus Erythematosus Disease Activity Index 2000 (SLEDAI-2K) and systemic Lupus International Collaborating Clinics/American College of Rheumatology Damage Index (SDI) respectively. Information on socio-demographics, clinical variables (SLEDAI-2K and SDI), co-morbidities (dyslipidemia, atherosclerosis, cerebrovascular disease, and others) are collected as part of the and will be made available for the analysis in this study. Lupus serology (including C3/C4, anti-ds DNA antibodies) and routine blood test (including complete blood count test and chemistry panel) are also collected regularly during the patients' visits to the clinic and will be made available for the analysis in this study.

fMRI Tasks: Participants will complete a series of questionnaires completed within 24 hours after the visit via Qualtrics and a series of tasks while functional MRI data is recorded. After the fMRI, there will be four cognitive tasks done on the computer outside of the scanner. These include:

Continuous Associative Binding (CAB): The goal of this task is to track different aspects of memory and decision-making, in particular the ability of individuals to form associations between pairs of items presented at the same time. In the tasks, participants are presented with pairs of images of objects (e.g., a pencil and a lamp) and their job is to indicate whether the have seen that exact pair of images presented together in the present block of trials.

Flanker: The goal of the flanker task is to measure inhibitory control and decision-making. In each trial, participants are presented with a cluster of arrows pointing either left or right. The task is for the participant to indicate the direction the arrow in the center of the cluster of arrows is pointing.

Random Dot Motion (RDM): The goal of this task is to track attention and perceptual decision-making. In each trial, participants see a circle filled with dots moving in different directions. Most of the dots are moving in random directions, but some of the dots are moving coherently either left or right. The task of the participant is to indicate (either by the keyboard or touch screen) whether more coherent dots are moving to the right or left.

Balloon Analog Risk Task (BART): The goal of this task is to track risk-taking behavior, reinforcement learning, and decision-making. On each trial, the participant indicates whether they would like to pump more air into the balloon, increasing the amount of points/money they could earn if they collect before the balloon pops, or whether they want to collect what they have earned and add it to the bank. If they pump and the balloon pops, they lose the chance to collect that money for that balloon.

Support people will complete a series of questionnaires completed within 24 hours after the visit via Qualtrics and the Handholding Task. The support person is the partner and will be asked to hold hands with the patient for the partner portion of the task. The support person will be connected to the shock device (STM100C Stimulator Module, BIOPAC Systems) for one round of the task, and the shock level will be calibrated to their pain tolerance.

After the fMRI, there will be four cognitive tasks done on the computer outside of the scanner. These include the same tasks for the participant (listed above).

For the scan, standard procedures for removal of all participant ferromagnetic objects (e.g., wristwatches) will be implemented, and the procedures of the study will be reviewed, insuring that participants have an opportunity to ask any remaining questions. All standard fMRI safety screening procedures will be done prior to the fMRI, and female participants will take a urine based pregnancy test. Participants will complete the following tasks while in the scanner:

Resting State Task: Mindfulness training has been shown to alter resting state connectivity in areas related to emotions and stress (e.g., Taren et al., 2015). Thus, we will record resting state data in all visits. Participants will be asked to rest in the scanner. Following the resting state scans, participants will also complete selected questions from the Amsterdam Resting State Questionnaire 2.0 to provide subjective descriptions of their experience.

Hand holding Task: The handholding task is a measure the social regulation of the neural response to threat. Each trial involves the presentation of 12 threat and 12 safety cues in randomized order across blocks of approximately 7 minutes. Participants and partners will be told that threat cues indicate a 17% chance of mild electric shock. These basic threat paradigms will be repeated across 3 blocks of threat/safety cues and counterbalanced across subjects. These blocks will include the alone condition, and the partner hand holding condition in the Threat to Self task, and the partner hand holding condition in the Threat to Partner task. Electric shock will be delivered via an automated computer controlled device (STM100C Stimulator Module, BIOPAC Systems) to the ankle (4 mA, cf., Tursky & O'Connell, 1972). The shock level will be calibrated to each participant's pain tolerance.

Resting State Task (a second time)

All fMRI conditions will be followed by ratings using the Self-Assessment Manikins.

ANALYSIS: The main analysis is planned when all patients have concluded the MBI or psychoeducational program, all data have been entered, verified and validated and the primary database has been locked. Following data reduction and preparation, analysis of all self-report and biological (e.g., fMRI) data will be conducted using hierarchical multilevel modeling procedures designed to maximize sensitivity to both within- and between- subject sources of variation across time, including baseline measurements pre- and post- intervention. In addition to testing for specific group-level effects of intervention, individual differences in response to treatment and/or in biological measures will be assessed as a function of self-report data at both state and trait levels, modeled as interaction effects in multilevel models.

Study Type

Interventional

Enrollment (Anticipated)

50

Phase

  • Not Applicable

Contacts and Locations

This section provides the contact details for those conducting the study, and information on where this study is being conducted.

Study Contact

Participation Criteria

Researchers look for people who fit a certain description, called eligibility criteria. Some examples of these criteria are a person's general health condition or prior treatments.

Eligibility Criteria

Ages Eligible for Study

18 years and older (Adult, Older Adult)

Accepts Healthy Volunteers

Yes

Genders Eligible for Study

All

Description

Inclusion Criteria:

  • Males and females who have given written informed consent
  • 18 years of age or older
  • Literate in English: able to read, understand, follow instructions, and complete the rating scales and questionnaires accurately
  • Have a clinical diagnosis of systemic lupus erythematosus
  • Must pass the initial MRI screening
  • Must be a participant in The University of Toronto Clinic and Database Research Program - Prognosis and Genetic Studies in Systemic Lupus Erythematosus
  • Must be able to access the Internet regularly

Exclusion Criteria:

  • Significant previous mindfulness training and experience (e.g. MBSR course, daily meditation practice)
  • Any current Axis I DSM-IV-TR psychiatric disorder that, in the clinician's opinion, warrants treatment or would preclude safe participation in the protocol, including, but not limited to: psychosis, schizophrenia, dementia, schizotypal personality disorder, borderline personality disorder, bipolar disorder, primary diagnosis of eating disorder, or chronic suicidality or homicidality.
  • Have clinical evidence of significant unstable or uncontrolled acute or chronic diseases not related to SLE (i.e., diabetes, cardiovascular, pulmonary, hematologic, gastrointestinal, neurological, or infectious) which, in the opinion of the treating physician, could confound the results of the study or put the patients at undue risk.
  • Chronic use of prescribed or recreational psychoactive drugs (self-reported)
  • Current drug or alcohol abuse or dependence, or a history of drug or alcohol abuse or dependence within 364 days prior to Baseline (self-reported)
  • Too sick to meaningfully participate (e.g. hospitalized, flaring at the time of screening)
  • In order to participate in the MRI portion of the study, participants must pass the in-person MRI screening administered by the MRI technician before each MRI. If participants fail the in-person MRI screening, they will be excluded from the MRI portion of the study, but can still participate in the intervention portion of the study.
  • Is not a participant in The University of Toronto Clinic and Database Research Program - Prognosis and Genetic Studies in Systemic Lupus Erythematosus

Study Plan

This section provides details of the study plan, including how the study is designed and what the study is measuring.

How is the study designed?

Design Details

  • Primary Purpose: Basic Science
  • Allocation: Randomized
  • Interventional Model: Parallel Assignment
  • Masking: Single

Arms and Interventions

Participant Group / Arm
Intervention / Treatment
Experimental: Mindfulness Intervention
Participants in this arm will participate in the Contemplative-Based Intervention for People Living with SLE intervention in addition to one baseline fMRI and blood analysis and one post-treatment fMRI and blood analysis.
Intervention sessions will follow a 6-week format consisting of weekly in-person sessions as well as guided homework to encourage practice at home. Some mindfulness practices that will be included are meditation, group exercise (yoga), group discussions, and deep breathing. Both participants diagnosed with SLE as well as caregivers will participate in the intervention sessions. 5 sessions will be approximately 2 hours long, while the final session will be approximately 4 hours long. Each intervention group will include approximately 4 participants with SLE and 4 caregivers.
Active Comparator: HEP Intervention
Participants in this arm will participate in the Health Enhancement Program (HEP) intervention in addition to one baseline fMRI and blood analysis and one post-treatment fMRI and blood analysis.
The HEP was designed to create an active control for mindfulness-based stress reduction (MBSR) interventions. The structure of this intervention will mirror that of the other arm of this study, but will lack the mindfulness component. The HEP includes topics such as physical activity, functional movement, music therapy, and nutrition education.

What is the study measuring?

Primary Outcome Measures

Outcome Measure
Measure Description
Time Frame
Change from baseline in systemic lupus erythematosus (SLE) disease activity
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline SLE Disease Activity Index 2000 (SLEDAI-2K) total score (range from 0 to 105 with higher values representing worse outcomes). Total score represents the sum of the central nervous system, vasculitis, musculoskeletal, renal, skin, serosal, immunologic, fever, and hematologic subscales.
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention

Secondary Outcome Measures

Outcome Measure
Measure Description
Time Frame
Change from baseline in brain activity during functional MRI
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change in brain activity during functional MRI handholding task
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in organ-specific SLE disease activity (central nervous system subscale)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in SLEDAI-2K central nervous system score (range 0-56 with higher values representing worse outcomes).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in organ-specific SLE disease activity (vasculitis subscale)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in SLEDAI-2K vasculitis score (range 0-8 with higher values representing worse outcomes).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in organ-specific SLE disease activity (musculoskeletal subscale)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in SLEDAI-2K musculoskeletal score (range 0-8 with higher values representing worse outcomes).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in organ-specific SLE disease activity (renal subscale)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in SLEDAI-2K renal score (range 0-16 with higher values representing worse outcomes).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in organ-specific SLE disease activity (skin subscale)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in SLEDAI-2K skin score (range 0-6 with higher values representing worse outcomes).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in organ-specific SLE disease activity (serosal subscale)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in SLEDAI-2K serosal score (range 0-4 with higher values representing worse outcomes).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in organ-specific SLE disease activity (immunologic subscale)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in SLEDAI-2K immunologic score (range 0-4 with higher values representing worse outcomes).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in organ-specific SLE disease activity (fever subscale)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in SLEDAI-2K fever score (range 0-1 with higher values representing worse outcomes).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in organ-specific SLE disease activity (hematologic subscale)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in SLEDAI-2K hematologic score (range 0-2 with higher values representing worse outcomes).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in erythrocyte sedimentation rate (ESR)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for ESR (mm/hr)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in antinuclear antibodies (ANA)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for ANA titer
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in white blood cell count (WBC), red blood cell count (RBC), platelet levels, and nucleated RBC count
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for WBC, RBC, platelet levels and nucleated RBC count (amount per microliter)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in hemoglobin levels and mean corpuscular hemoglobin concentration (MCHC)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for hemoglobin levels and mean corpuscular hemoglobin concentration (MCHC) (g/dL)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in hematocrit levels, red cell distribution width (RDW), and nucleated red blood cell percentage
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for hematocrit levels, RDW, and nucleated red blood cell percentage (%)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in mean corpuscular volume (MCV) and mean platelet volume (MPV)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for MCV and MPV (fL)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in mean corpuscular hemoglobin (MCH)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for MCH (pg)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in blood sodium, potassium, chloride, carbon dioxide, and anion gap (mmol/L)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for baseline in blood sodium, potassium, chloride, carbon dioxide, and anion gap (mmol/L)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in blood urea nitrogen, creatinine, glucose, and calcium levels
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for blood urea nitrogen, creatinine, glucose, and calcium levels (mg/dL)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in high sensitivity C-reactive protein (CRP)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for CRP (mg/L)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in complement C3 and complement C4
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for complement C3 and complement C4 (mg/dL)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in cytokine panel (tumor necrosis factor alpha; interleukin 2, 2 receptor (CD25) soluble, 12, gamma, 4, 5, 10, 13, 17, 1 beta, 6, 8)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Abnormal lab values for cytokine panel (pg/mL)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Adult attachment style questionnaire - closeness subscale (AAS)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in AAS scores (range from 6-30 with higher scores indicating better outcomes)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Adverse childhood experiences questionnaire (ACE)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in ACE scores (ranging from 0-10 with higher scores suggesting worse outcomes)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Brief Health Mindset Scale (BHMS)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in BHMS scores (ranging from 6-36, with higher scores reflecting more adaptive mindsets about health)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Center for Epidemiological Studies Depression Scale (CESD-R)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in CESD-R scores (ranging from 0-80 with higher scores representing worse outcomes. Sum of sadness/dysphoria, loss of interest/anhedonia, appetite, sleep, thinking/concentration, guilt/worthlessness, tired/fatigue, movement/agitation, suicidal ideation subscales).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Inclusion of Other in Self Scale (IOS)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in IOS scores (ranging from 1-7 with higher scores representing more relationship closeness)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Interpersonal Reactivity Index (IRI)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in IRI scores (ranging from 0-112 with higher scores indicating higher empathy. Sum of empathic concern, perspective-taking, fantasy, and personal distress subscales).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Interpersonal Regulation Questionnaire (IRQ)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in IRQ scores (ranging from 16-112, with higher scores reflecting better outcomes. Total score is sum of negative-tendency, negative-efficacy, positive-tendency, and positive-efficacy subscales.)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
MacArthur Scales of Subjective Social Status (community ladder)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in MacArthur Scales of Subjective Social Status (community ladder score ranging from 1-10 with higher scores indicating better outcomes)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
MacArthur Scales of Subjective Social Status (socioeconomic status ladder)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in MacArthur Scales of Subjective Social Status (socioeconomic status ladder score ranging from 1-10 with higher scores indicating better outcomes)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Caregiver Burden Questionnaire (CBQ)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in CBQ scores (ranging from 0-88 with higher scores representing worse outcomes)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Multidimensional Scale of Perceived Social Support (MSPSS)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in MSPSS scores (ranging from 12-84 with higher scores indicating better outcomes. Sum of family, friends, and significant other subscales)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Pain Catastrophizing Scale (PCS)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in PCS scores (ranging from 0-52 with higher scores representing worse outcomes. Sum of rumination, magnification, and helplessness subscales)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Ruminative Responses Scale (RRS)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in RRS scores (ranging from 10-40 with higher scores representing worse outcomes. Sum of brooding and reflection subscales).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Social Interaction Phobia Scale (SIPS)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in SIPS scores (ranging from 0-56 with higher scores representing worse outcomes. Sum of social interaction anxiety, fear of overt evaluation, and fear of attracting attention subscales).
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
State Trait Anxiety Inventory (STAI)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in STAI scores (ranging from 40-160 with higher scores representing worse outcomes. Sum of trait anxiety and state anxiety subscales)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Ten Item Personality Inventory (TIPI)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in TIPI scores on each of conscientiousness, openness to experience, extraversion, agreeableness, and neuroticism personality traits (ranging from 1-7 on each personality trait with higher scores representing more expression of each personality trait.)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Toronto Mindfulness Scale (TMS)
Time Frame: Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention
Change from baseline in TMS scores (ranging from 0-52 with higher scores representing greater mindfulness. Sum of curiosity and decentering subscales)
Baseline Assessment within 2 weeks prior to intervention, within 2 weeks after intervention

Collaborators and Investigators

This is where you will find people and organizations involved with this study.

Investigators

  • Principal Investigator: William A Cunningham, PhD, University of Toronto

Study record dates

These dates track the progress of study record and summary results submissions to ClinicalTrials.gov. Study records and reported results are reviewed by the National Library of Medicine (NLM) to make sure they meet specific quality control standards before being posted on the public website.

Study Major Dates

Study Start (Anticipated)

January 1, 2020

Primary Completion (Anticipated)

July 1, 2021

Study Completion (Anticipated)

July 1, 2021

Study Registration Dates

First Submitted

June 27, 2019

First Submitted That Met QC Criteria

July 22, 2019

First Posted (Actual)

July 25, 2019

Study Record Updates

Last Update Posted (Actual)

December 20, 2019

Last Update Submitted That Met QC Criteria

December 19, 2019

Last Verified

December 1, 2019

More Information

Terms related to this study

Other Study ID Numbers

  • 34709

Plan for Individual participant data (IPD)

Plan to Share Individual Participant Data (IPD)?

NO

Drug and device information, study documents

Studies a U.S. FDA-regulated drug product

No

Studies a U.S. FDA-regulated device product

No

This information was retrieved directly from the website clinicaltrials.gov without any changes. If you have any requests to change, remove or update your study details, please contact register@clinicaltrials.gov. As soon as a change is implemented on clinicaltrials.gov, this will be updated automatically on our website as well.

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