IBD Clinical Trial
Official title:
Identifying a Sleep Screener for Disease Relapse in Children With Inflammatory Bowel Disease
Background: Inflammatory bowel disease (IBD) is a group of disorders characterized by
chronic inflammation of the gastrointestinal tract with remissions and relapses. The two
most common subtypes are Crohn's disease (CD) and ulcerative colitis (UC). In 2012, the
burden-of-illness report from the Crohn's and Colitis Canada estimated that the direct
medical costs of IBD in Canada were over one billion dollars, primarily funded through the
Canadian public healthcare system.
Many life style-related factors may play an important role in the pathogenesis of IBD and
can contribute to trigger disease relapse, but several of these factors are poorly
understood. These factors may include sleep disturbances. Data on sleep disturbance in
children with IBD are limited. Sleep deprivation has been shown to cause reactivation of
colitis in animal studies but similar data are lacking in humans especially in children.
Hypothesis: In children with IBD, high scores for a sleep disturbance screener will be
positively associated with IBD relapse Objective: To develop a non-invasive non-costly tool
to screen for relapses in pediatric IBD patients through examining the association between
sleep disturbances and disease relapse in children with IBD Methods: This study will
incorporate an observational prospective design. Participants: Participants will be 90
children (ages 8-17 years ) under the care of the Pediatric IBD Program at the Children's
Hospital, Winnipeg. All participants will have an established diagnosis of IBD.
Measures: Sleep disturbances will be assessed using a sleep diary. Patients will be asked
complete a daily sleep diary in the week preceding their clinic appointment. The sleep diary
will provide information about latency to fall asleep, number of awakenings, duration of
awakenings, total sleep time, sleep quality, and sleep efficiency.
Mucosal inflammation will be assessed by measuring fecal calprotectin and clinical disease
activity will be measured Pediatric Crohn's disease activity index (PCDAI) for CD and
pediatric ulcerative colitis activity index (PUCAI) for UC at clinic visits
Anxiety/Depression: As anxiety and depression are often comorbid with disturbed sleep,
levels of symptoms in both domains will be assessed at clinic visit using the Child and
Parent Report Versions of the Spence Anxiety Scale and the Child Depression Inventory (v.
2).
Procedure: Upon obtaining informed consent, each participant will complete 7 days of sleep
diary recording in the week prior to their clinic appointment. During the clinic visit, the
PCDAI or PUCAI, Spence Anxiety Scales, Child Depression Inventory will be completed. Fecal
samples will be collected for fecal calprotectin measurement as a surrogate marker for
mucosal inflammation. Other investigations will include blood samples for serum hemoglobin,
serum albumin, and inflammatory markers. Stool samples for infection screen will also be
collected to exclude any possibility for gastrointestinal infection on top of IBD.A second
clinic visit will be scheduled 3 months later and the whole process will be repeated in the
second visit.
Regression analysis will be performed to examine the association between sleep disturbances
and disease activity, characteristics and patients' demographics
Outcomes:
Primary outcome: Cut-off score of a sleep screener that is associated with disease relapse
(as diagnosed by fecal calprotectin value of >100 microgram/gram of stools) in children with
IBD Secondary outcomes: 1. Correlation between sleep disturbance scores and clinical disease
activity indices (PCDAI and PUCAI). 2. Identification of which sleep component (sleep
duration, latency, fatigue, subjective quality) is the best at detecting a disease relapse.
3.Identification of whether sleep disturbance more accurately predicts relapse for CD than
for UC.
Hypothesis: In children with IBD, high scores for a sleep disturbance screener will be
positively associated with IBD relapse
Project Design and Specific Objective: This is a single centre pediatric observational
prospective study to develop a non-invasive non-costly tool to screen for relapses in
pediatric IBD patients through examining the association between sleep disturbances and
disease relapse in children with IBD. The outcomes are
Primary outcome: Cut-off score of a sleep screener in relation to disease relapse (as
diagnosed by fecal calprotectin value of >100 microgram/gram of stools) in children with IBD
Secondary outcomes
1. Correlation between sleep disturbance scores and clinical disease activity indices
(PCDAI and PUCAI), after controlling for symptoms of anxiety and depression
2. Identification of which sleep component such as sleep duration and sleep latency is the
best at detecting a disease relapse.
3. Identification of whether sleep disturbance more accurately predicts relapse for CD
than for UC, after controlling for symptoms of anxiety and depression.
4. Identifying any differences in intestinal microbiom between those with sleep
disturbances versus those without.
Experimental Methods and Analysis
1 Design: Observational prospective study 2. Inclusion Criteria 2.1. Children aged 8 -17
years under the care of the Pediatric IBD Program at the Children's Hospital, Winnipeg and
with an established diagnosis of IBD according to the North American Society of Pediatric
Gastroenterology (NASPGHAN) 3. Exclusion Criteria 3.1. Children with IBD and known cognitive
dysfunction or global developmental delay 3.2. Children with IBD and concurrent
gastrointestinal infection 4 Measures
- 4.1. A standardized sleep diary will assess sleep in the past week. Scores will be
averaged over the 7-day recording period. The sleep diary will provide information
about latency to fall asleep, number of awakenings, duration of awakenings, total sleep
time, sleep quality, and sleep efficiency. To complement the sleep diary, the
Children's Report of Sleep Patterns, a 62-item questionnaire, will assess self-reported
sleep patterns, sleep hygiene, and sleep disturbance in children ages 8-17 years. It
has acceptable reliability and validity.
- 4.2. Disease relapse will be measured using fecal calprorectin (F Cal) and the PCDAI
for CD and PUCAI for UC.The quantum blue single point of care test (ALPCO) will be used
- 4.3. The disease phenotype, duration, base-line characteristics, patient demographics,
smoking habits, medications, and initiation of new medications or other treatments for
IBD during the course of the study will be obtained by chart review using an
information form
- 4.4. The Spence Children's Anxiety Scale will be used to assess anxiety symptoms (e.g.,
panic attacks, social phobia, fear of physical injuries, generalized anxiety). With
clinical cut-offs, the scale has demonstrated high internal consistency and good
test-retest reliability over a six-month period. Evidence of convergent and divergent
validity has been reported. As parent and youth report can differ, both self-report and
parent-report versions of the SCAS will be administered.
- 4.5. The Child Depression Inventory -II (short-form) is a 12-item scale of depressive
symptoms for youth aged 7 to 17 years. It represents one of the most widely used
measures of depression in this age group, has excellent reliability, concurrent,
construct, and predictive validity. Both self-report and parent-report will be
collected.
5. Study procedure: Families with children aged 8 -17 years, who are under the care of
the Pediatric IBD Program at the Children's Hospital, Winnipeg, and who have an
established diagnosis of IBD will be approached via letters to inform them about the
study and study procedures. The letters will give the option to patients and their care
givers to declare their lack of interest in participation if they do not want to be
approached or participate in the study. Patients and parents/guardians/care givers will
choose whether or not to provide "permission to be contacted via phone". This will
occur through a phone number provided in the letter, and they will be instructed to
call within 1 week of receiving the letter to declare if they decline to be approached.
If lack of interest is not declared, the Research Assistant will call the potential
participants to explain the study procedure, obtain a verbal consent for participation
and ask participants to complete a sleep diary to assess sleep disturbances for one
week prior to the clinic visit. During the clinic visit, verbal consent will be
confirmed and informed assent/consent will be obtained by the children/parents
(guardians) and the completed sleep diary will be collected. During the same visit,
fecal samples will be collected for FCAL measurement as a surrogate marker for mucosal
inflammation. A fecal sample will be laso sent for microbiome analysis. Other
investigations will include blood samples for serum hemoglobin, serum albumin, and
inflammatory markers (CRP and ESR) and if participants have diarrhea, stool samples for
infection screen will be collected to exclude any possibility for gastrointestinal
infection. In addition, participants and their parents will complete the Spence Child
Anxiety Scale, the Child Depression Inventory (parent and child report), and the
Children's Report of Sleep Patterns (CRSP)(child report). It is expected that
administration of these measures during clinic will take 45 minutes. The Research
Assistant will help participants who need any clarification on how to respond to any
question. Children will also be clinically assessed and clinical disease activity will
be measured using PCDAI for CD and PUCAI for UC. Each participant will have all
measures repeated at a second elective clinic visit 3 months later during the course of
the study period (9 months of recruitment). Patients are normally instructed to call
our office if they start developing symptoms of relapse such as diarrhoea and abdominal
pain. Patients then will be asked over the phone to complete a sleep diary and to bring
a stool sample for fecal calprotectin. Stool samples for infection screen will be also
collected and an emergency clinic visit for clinical assessment of the disease and
routine blood tests including blood samples for measuring inflammatory markers will be
planned within a week of having symptoms of relapse. Completed sleep diary will be
collected during the visit.
5. Analysis and sample size To determine whether sleep disturbance is associated with
disease relapse, logistic regression analysis will be conducted. Logistic regression
will be used as the goal of the analysis is to predict the category of outcome for
individual patients (relapsed, not relapsed). As symptoms of anxiety and depression are
often comorbid with sleep disturbance, we will use these as covariates in the logistic
regression analysis.
To determine the diagnostic performance of the sleep measures, or the level of sleep
disturbance associated with disease relapse, ROC will be analyzed using MedCalc. MedCalc is
a reliable and valid method of assessing the diagnostic validity of laboratory tests. ROC
curve analysis methodology will be used to plot curves representing the true positive (TPR)
and false positive rates (FPR) for sleep at different cut-off points. ROC curves will be
used in this investigation to determine an optimal cutoff level for the sleep measures and
to contrast the relative adequacy of measures to discriminate between participants who
relapsed versus those who did not. The MedCalc program assumes an underlying bi-normal
distribution and produces a non-parametric estimation of the area under the curve. Results
from the PCDAI and PUCAI will be the reference standard for the test. Information pertaining
to test, specificity, positive predictive value (PPV, and negative predictive value (NPV
will be obtained. Such an analysis will produce a range of sensitivity and specificity
values associated with different cut-off points for each of the sleep variables and the
MedCalc program chooses a cutoff point that maximizes both sensitivity and specificity.
Using a corrected z-test, analogous to a paired t-test, results will show whether there is a
statistically significant difference between the sleep predictors in terms of the overall
accuracy of measurement.
Based on existing studies of sleep disturbances in IBD, sleep disturbances are assumed to be
prevalent in 80% of patients with active IBD compared to 40% of those in remission. To
achieve an acceptable power of .80 with alpha = .05, a sample of 90 patients will be
recruited. This number is highly feasible to recruit within the proposed clinic's patient
flow and where research participation rates exceed 80% in the current and past research
projects in the pediatric IBD program. Currently the IBD program cares for over 150 children
with IBD with over 130 patients > 8 years old.
Descriptive analyses of the variables will be performed comparing disease type (CD/UC) and
disease status (inactive (F Cal < 100 microgram/gram stools /active (F Cal > 100
microgram/gram of stool)). Comparisons of disease subtypes and active/inactive subgroups
will be performed using two-tailed t-tests for continuous variables, and chi-square/Fisher
exact tests of association for categorical variables.
;
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Withdrawn |
NCT04269720 -
Biofeedback in Pediatric Inflammatory Bowel Disease
|
N/A | |
| Recruiting |
NCT04457934 -
Effectiveness of PLENVU in the General Screening Population and Patients With IBD
|
||
| Completed |
NCT01369355 -
A Study to Evaluate the Safety and Efficacy of Ustekinumab Maintenance Therapy in Patients With Moderately to Severely Active Crohn's Disease (IM-UNITI)
|
Phase 3 | |
| Recruiting |
NCT06146816 -
The Assessment of Infrared Treatment for Crohn's Disease
|
N/A | |
| Recruiting |
NCT05624801 -
Cholecalciferol in Chronic Inflammatory Bowel Diseases
|
Phase 3 | |
| Recruiting |
NCT05086562 -
Prevalence of Chronic Abdominal Pain in Migraneurs
|
||
| Recruiting |
NCT03935451 -
Postoperative Extended Venous Thromboprophylaxis in Inflammatory Bowel Disease
|
Early Phase 1 | |
| Recruiting |
NCT05578768 -
Prediction of IBD Disease Activity in Individual Patients Based on PROMs and Clinical Data
|
||
| Completed |
NCT01653054 -
Anal Dysplasia in Patients With Inflammatory Bowel Disease
|
N/A | |
| Completed |
NCT04131504 -
Precision Crohn's Disease Management Utilizing Predictive Protein Panels (ENvISION)
|
||
| Recruiting |
NCT03952364 -
The PRECIOUS Study: Predicting Crohn's & ColitIs Outcomes in the United States
|
||
| Enrolling by invitation |
NCT05414955 -
Boom-IBD Clinical Trial
|
N/A | |
| Enrolling by invitation |
NCT04094324 -
Mental Health in Children and Youth Within Pediatric Care
|
||
| Suspended |
NCT04225819 -
Adjunctive Treatment With Vitamin D3 in Patients With Active IBD
|
N/A | |
| Recruiting |
NCT03366090 -
Immunological Profiles in Inflammatory Bowel Disease
|
N/A | |
| Completed |
NCT03750565 -
Multiple Dose Ethnobridging PK Study in Healthy Subjects
|
Phase 1 | |
| Completed |
NCT02622139 -
Multispectral Optoacoustic Tomography (MSOT) for the Evaluation of Disease Activity in Inflammatory Bowel Diseases (IBD)
|
N/A | |
| Completed |
NCT02364973 -
Combined PET-MRI in the Diagnostics of Chronic Inflammatory Bowel Diseases (IBD)- a Feasibility Study
|
||
| Not yet recruiting |
NCT06090045 -
Airway Involvement In Inflammatory Bowel Disease
|
||
| Not yet recruiting |
NCT06089590 -
Ibd CAncer and seRious Infections in France (I-CARE 2)
|