Irritable Bowel Syndrome (IBS) Clinical Trial
Official title:
Confocal Endomicroscopy Utility for Diagnosing Mucosa Micro-inflammation in Patients With Irritable Bowel Syndrome
Irritable bowel syndrome (IBS) is one of the most common gastrointestinal disorders. It has
prevalence in general population of 5-20% and is more common in women and young adults.
Despite being one of the most frequent reasons for consultation many patients are
undiagnosed. There are no reliable biomarkers. The diagnosis is clinical, based on the Rome
III criteria. IBS is characterized by chronic or recurrent abdominal pain associated with
changes in bowel frequency and consistency, when other etiologies are excluded. The
combination of the Rome III criteria with the absence of alarm symptoms have a sensitivity of
65%, specificity of 100%, 100% positive predictive value and negative predictive value of
76%.
Current tests commonly fail to obtain an objective diagnosis, and effective therapies are
lacking. There are no specific endoscopic findings that can discriminate IBS patients from
healthy patients. Most colonoscopies are performed to rule out other etiologies and in more
than 50% of the cases are normal.
The pathophysiology is complex, multifactorial and not completely known. Impaired intestinal
barrier function and mucosal inflammation in the small and large intestine have been
reported. Evidence of inflammation and neuronal degeneration in the myenteric plexus has been
found in full-thickness intestinal biopsy samples from IBS patients.
It has been found that IBS patients had a significantly higher density of intestinal
epithelial gaps. The elevated epithelial gaps in the intestine of IBS patients, a surrogate
marker for increased epithelial cell extrusion, may be a cause of altered intestinal
permeability observed and may lead to mucosal inflammation.
Confocal laser endomicroscopy (CLE) is a new endoscopic imaging tool enabling visualization
of changes in the gut mucosa. The use of intravenous fluorescein enables high-resolution
real-time imaging in vivo at a micron scale, allowing visualization of cellular details
during ongoing endoscopy. This technology can be used to identify and quantify epithelial
gaps and other signs of inflammation.
The purpose of this study is to evaluate the presence of microscopic inflammation previously
demonstrated in patients with IBS, using pCLE. The determination of the exact areas of
inflammation allows a direct biopsy in a more accurate way. This type of systematic may allow
in the future to classify these patients not only symptomatically (constipation, diarrhea or
mixed predominant IBS) but also according to their degree of inflammation. There is no Gold
Standard test in these patients to assess response to treatment. The possibility of using
pCLE to identify the areas of microscopic inflammation allows that the degree of inflammation
can be used as a monitoring parameter. Probably the CLE can be used to assess response to
treatment and different types of treatments, determining differences between subtypes of
patients with IBS, evaluate remission, recurrence and prognosis. Also it may clarify a
potential mechanism of the pathogenesis and be endoscopic criteria for the diagnosis of the
disease.
The present study is the first to evaluate the colon microscopic inflammation using pCLE in
IBS patients.
Study design: This is an observational and analytical cross-section, population - based
survey study, with prospective case collection, non-randomized and simple blind, performed in
a Tertiary Academic Center.
Setting: Ecuadorian Institute of Digestive Diseases (IECED), OmniHospital Academic Tertiary
Center. We will include patients from October 2015 to March 2016. Patients will be recruited
from the gastroenterology unit (IECED). The study protocol and consent form has been approved
by the Institutional Review Board (IRB) and will be conducted according to the declaration of
Helsinki. Patients will sign an informed consent and answer a questionnaire that includes
constitutional data (sex, age, comorbid medical condition, medication). Patients in IBS group
will be classified according to the symptoms as diarrhea predominant (IBS-D), constipation
predominant (IBS-C) or mixed type (IBS-M). Endoscopic findings will be recorded in a
database.
Endoscopic technique: All colonoscopies will be performed after the patient had undergone
standard bowel preparation using either polyethylene glycol electrolyte lavage solution.
Initially a routine white light colonoscopy will be performed in IBS and healthy control
patients, using a Pentax scope (Pentax EC-387CILK, Tokyo, Japan) with great care not to
damage the epithelium. The Boston Bowel Preparation Scale and inflammation changes will be
recorded.
During withdrawal, all parts of the colon will be evaluated (cecum, right-side colon,
transverse, left-side colon, sigmoid and rectum) using pCLE randomly in one point of each
segment, if there are no signs of iatrogenic mucosal damage. Careful washing of the mucosa
with water in order to prevent the inclusion of image artefacts from residual stool
fragments. Before initiating CLE evaluation, intravenous injection of 5 ml 10% fluorescein
will be done. Fluorescein stains vessels and gives good tissue structure, but the nuclei are
not stained and appear as dark spots. Optimal contrast is obtained within the first 10min
after injection, but good quality images can be acquired for a further 30-60 min.
Currently Confocal Laser Endomicroscopy (CLE) is performed using a CLE probe (pCLE). The
confocal microscope used in pCLE captures microscopic images of untreated in vivo tissue. The
microscope uses focused laser light of a defined wavelength and passes it through a confocal
aperture. Images are then reconstructed in two dimensions. For pCLE (Cellvizio by Mauna Kea
Technologies, Paris, France), both the laser scanning unit and light source are outside the
body. The laser beam is transported via flexible confocal miniprobes and a distal lens
sequentially scans it through a bundle of more than 10000 optical fibers. Confocal miniprobes
are flexible, with diameters ranging from 0.9 mm to 2.5 mm.
In the study a pCLE ColoFlex probe will be used (Cellvizio; Mauna Kea Technology, Paris,
France). The probe goes through the accessory channel of a conventional endoscope. The image
rate is 0.08 s/frame at 1024×1024 pixels with a imaging depth of 20 μm. The confocal images
will be first analyzed during the endoscopy. Then, the images will be digitally stored and
reviewed after the procedure in order to zoom in on details for a higher magnification
(approximately 10000 fold), with special designed software package (Cellvizio Viewer),
allowing image correction and stabilization.
Immediately after pCLE evaluation, and before proceeding to the next colon segment, targeted
biopsies will be taken from the mucosal area evaluated. Bleeding can impair image quality,
therefore probe will be placed gently in contact with the tissue in order to avoid trauma and
pCLE imaging will be completed in a region before mucosa biopsy. The endoscopist performing
the pCLE will be blinded to the status of the patient and the images will be later analyzed
in detail blindly by two different persons with more than two years' experience in
endomicroscopy.
There are not studies that validate a classification of colon inflammation using CLE in IBS
patients. Inflammation of the colon mucosa in ulcerative colitis (UC) has been described
previously using CLE. Kiesslich et al. reported on a 3-grade classification of inflammation
activity by CLE, combining crypt architecture, cellular infiltrations, and vessel
architecture. Nevertheless the assessment of cellular infiltration has been questioned
because of the difficulty in differentiating cell types by CLE. Chang-Qing Li, et al. used
three CLE parameters to evaluate inflammation in UC patients: a 4-grade crypt-architecture
classification, fluorescein leakage, and microvascular alterations. On the other hand, the
Miami classification for pCLE defines colitis using: crypt fusion and distortion, bright
epithelium, dilated and prominent branching vessels.In the present study the parameters used
for CLE inflammation will be: 1.Epithelial gaps followed by leaks with secretion of
fluorescein into the lumen. In CLE images of normal colonic mucosa, the lumen of the crypt is
free of fluorescein and appears as a dark center in the crypt; however, in inflamed mucosa,
fluorescein leaks into the crypt lumen; therefore, the lumen is brighter than the surrounding
epithelium. 2.4-grade crypt-architecture classification: Types A and B will be considered as
normal and chronic inflammation, respectively, and types C and D indicate acute inflammation.
Type A: Regular arrangement and size of crypts. Type B: Irregular arrangement of crypts,
enlarged spaces between crypts. Type C: Dilation of crypt openings, more irregular
arrangement of crypts, and enlarged spaces between crypts as compared to type B. Type D:
Crypt destruction and / or crypt abscess. 3.Dilated and prominent branching vessels
Interobserver and Intraobserver Agreement: A data set containing CLE photographs and videos
of the all of the colon segments will be presented to three blinded endoscopists, who will
confirm or not the findings. Inter- and intra-observer reproducibility will be measured based
on comparison of still images and videos between the three investigators. To evaluate the
intra-observer agreement each investigator will assess the images two times and the answers
will be compared. To evaluate the inter-observer agreement all answers between the three
investigators will be compared. In general, the learning curve of CLE is short and inter or
intra-observer agreement is good.
Statistical analysis: Baseline characteristics will be compared between case and control
group using Chi-square o Fisher Test for categorical variable, and for continuing variables,
we will use the Mann-Whitney Test. Diagnosis efficacy will be measured thought sensitive,
specificity and accuracy. All the statistical analysis will be performed using SPSS software
suite v.22.
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