Clinical Trial Details
— Status: Not yet recruiting
Administrative data
| NCT number |
NCT05407350 |
| Other study ID # |
USE-IT-01434 |
| Secondary ID |
|
| Status |
Not yet recruiting |
| Phase |
|
| First received |
|
| Last updated |
|
| Start date |
June 2022 |
| Est. completion date |
June 2025 |
Study information
| Verified date |
April 2022 |
| Source |
International Bowel Ultrasound Group e.V. |
| Contact |
Jimmi Cording, PhD |
| Phone |
004915129110689 |
| Email |
jc[@]bowel-ultrasound.org |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Observational
|
Clinical Trial Summary
The primary objective of this study is to prospectively validate a novel intestinal
ultrasound (IUS) Crohn's disease (CD) activity index and component items, correlating CD
activity and responsiveness to therapy as evaluated by IUS with evaluations by
ileocolonoscopy (IC) (Simple Endoscopic Score for Crohn's disease [SES-CD]) and magnetic
resonance enterography (MRE) (Simplified Magnetic Resonance Index of Activity [MaRIA] score).
Description:
Study Design Prospective multicenter study of 111 participants with CD with 50 weeks of
follow-up Study Population Adult patients with moderately to severely active CD
Inclusion Criteria:
1. Confirmed diagnosis of CD according to standard clinical, endoscopic, and histologic
criteria of at least 3 months duration
2. Adults 18 years of age or older
3. Moderate to severely active CD defined by:
1. Active symptoms with a HBI ≥ 8, and
2. Bowel wall inflammation defined as bowel wall thickness (BWT) > 3 mm in at least 1
segment of the ileum or colon as determined by IUS
4. Patients with planned introduction of biologic therapy as per their treating
gastroenterologist to treat active disease
5. Written informed consent must be obtained and documented
Exclusion Criteria:
1. Patients with a primary diagnosis of ulcerative colitis or IBD type unclassified
2. Patients with prior intestinal surgery
3. Patients with disease-related structural bowel complications, defined as either:
1. Stricture with increased bowel wall thickening (>25% of normal), decreased luminal
diameter (≥ 50% relative to the normal adjacent bowel loop) and proximal dilation
(on any imaging modality), or
2. Penetrating complications (excluding perianal fistulizing disease; patients with
perianal disease are eligible if there is additional inflammation in another bowel
segment [other than the rectum])
4. Contraindication to IC or MRE
5. BMI greater than 35 at time of screening or other characteristics considered likely to
preclude IUS visualization of all bowel segments
6. Disease limited to the rectum
7. Serious underlying disease other than CD that in the opinion of the investigator may
interfere with the participant's ability to participate fully in the study
8. History of alcohol or drug abuse that in the opinion of the investigator may interfere
with the participant's ability to comply with the study procedures
9. Pregnancy Data Sources and Data Collection Data will be collected from patient charts
(paper or electronic) including medical and CD related history, medication records, and
results of prior laboratory and imaging examinations. Patient disease-related outcomes
including hospitalizations, emergency department (ED) visits, and surgeries will be
collected during visits for analysis. Data will be transcribed from the patient's chart
and entered into an electronic case report form by the investigator or authorized
trained designee.
Questionnaires are to be completed by healthcare professionals and patients (i.e., baseline
demographics, HRQoL ]SIBDQ], PRO-2, IBD Knowledge Questionnaire).
Outcomes
Primary Outcome:
• The longitudinal and construct validity and treatment responsiveness of an IUS CD activity
index in an adult population with moderate to severely active CD
Secondary Outcomes:
- The correlation of IUS CD activity index and component items with IC
- The correlation of IUS CD activity index and component items with MRE
- The correlation of IUS CD activity index and component items with biomarkers
- The correlation of IUS CD activity index and component items with clinical activity
scores
- The correlation of IUS CD activity index and component items with histology
- The correlation of IUS CD activity index and component items with HRQoL (SIBDQ) and
PRO-2
- The proportion of patients with IUS response and transmural healing after initiation of
a biologic therapy approved for CD
- The longitudinal validity of changes in IUS CD activity and component items after
treatment with changes in IC, MRE, biomarkers, clinical disease activity scores, HRQoL
(SIBDQ), PRO-2, and histology
- The correlation of terminal ileal small bowel peristalsis with IUS CD activity index and
component items, MRE, and IC with CD activity
- The correlation of IUS CD activity index and component items with patient outcomes,
including ED visitation, hospitalization, and surgery.
Statistical Methods Demographic and clinical data will be evaluated using descriptive
statistics. A putative IUS CD activity index in development using at least moderately
reliable (inter-rater ICC > 0.40) items from a prior study (Part I) and its component items
will be evaluated in this prospective cohort study.
Sample Size:
Power calculations are based on the primary endpoint of IUS CD activity index responsiveness.
Based on the variance formula for the standardized mean change, and assuming a correlation of
0.3 for baseline and follow-up scores, a sample size of 94 paired scores would have 80% power
to detect a standardized mean change of 0.35. Accounting for 15% attrition, a sample size of
111 participants will be needed.
Outcome Analysis:
The primary aim of this study is to both establish IUS CD activity index responsiveness to
effective medical therapy with demonstration of changes in activity over time as well as
index external validation through correlation of individual IUS activity index components and
overall score compared to both IC and MRE.
Similar correlations will be examined between the IUS CD activity index and HBI, GHAS, RHI,
SIBDQ, PRO-2, transmural healing, terminal ileal small bowel peristalsis, and patient
outcomes including ED visitation, hospitalization, and surgery. All participants in this
prospective cohort will receive medical therapy of known efficacy for CD. The definition of
change will be based on a global IUS measure of disease activity, quantified using a 100 mm
visual analog scale (VAS), where 0 represents no disease activity and 100 represents the
worst disease activity ever seen. Clinically meaningful change will be defined by a decrease
of more than ½ the SD of the global IUS VAS at Baseline. Longitudinal validity will be
correlated with changes in the IUS CD activity index and other measures of disease activity
on IC, and changes in MRE (Simplified MaRIA score), HBI, CRP, and fCal. Responsiveness will
be quantified using the standardized effect size (mean difference divided by SD) and the
associated 95% CI, as well as the nonparametric probability for detecting change, expressed
as the AUROC. Weighted correlation coefficients will be used to quantify longitudinal
validity. An exploratory knowledge questionnaire (IBD Knowledge Questionnaire) will also be
used to evaluate the evolution of patient IBD understanding through study participation. The
potential for this study data to be applied in machine learning IUS diagnostics will also be
considered.
Expected Impact Development of a reliable and responsive IUS CD activity index will improve
standardization and consistency in IUS utilization globally. In the long-term, this can
profoundly change the way in which IBD care is delivered, with wider adoption of repeatable
accurate disease activity evaluation in clinic resulting in accelerated uptake of a
treat-to-target strategy in CD. This strategy has been demonstrated to better inform clinical
decision making, improve patient outcomes, and reduce long-term disability in patients with
CD. In addition, an increased IUS uptake can engage patients to better understand their
disease which will result in improved adherence to monitoring and treatment which will
ultimately improve CD related outcomes.
