Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT00816491 |
| Other study ID # |
08-PP-06 |
| Secondary ID |
|
| Status |
Completed |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
October 2008 |
| Est. completion date |
November 9, 2013 |
Study information
| Verified date |
May 2022 |
| Source |
Centre Hospitalier Universitaire de Nice |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
The primary endpoint of the study will be to compare the accuracy of two procedures (FICE
with target biopsies only, versus conventional white light colonoscopy with recommended
targeted and random biopsies) in the endoscopic surveillance of patient with long-standing
UC. Accuracy will be measured based on the number of patients with confirmed neoplasia using
each technique. The combined histological outcome following the two procedures will represent
the gold-standard diagnosis for each patient. Secondary outcomes will be the number of
patients with false-positive findings, the number of neoplastic lesions detected, the number
of false-positive lesions per patient for each technique and the total time required for each
procedure.
Description:
Patients will undergo two colonoscopies each, with an interval of three months between
procedures. This minimum time interval is chosen in order to allow for the healing of the
mucosa on sampled areas and thus prevent recognition of biopsy sites. The first procedure
will be randomly allocated to be either conventional white light endoscopy coupled with
targeted and random biopsies or high-resolution endoscopy with FICE system and magnification.
Randomisation will be achieved prior to the first endoscopy by means of sealed envelopes. In
each recruitment centre, one of the two endoscopists with experience in endoscopic
surveillance and treatment of ulcerative colitis will be assigned to carry out the first
procedure. The second procedure will automatically be scheduled with the second endoscopist,
who will be blinded as to the clinical and histological findings of the first investigation.
The two participating centres are already endowed with identical endoscopic equipment. All
examinations will be performed using the same high resolution endoscope (EC-590 ZW, Fujinon
Inc., Daitama, Japan). The zoom function on the device will only be used during the FICE
procedures. The system is equipped with the EPX 4400 processor (Fujinon Inc., Japan) that
enables the CVC technology. This digital processing system can switch between conventional
imaging and CVC imaging at any time during the procedure by means of a simple pushbutton on
the endoscope. The system has up to ten (# 10) settings designed to select the most suitable
wavelengths. In this study the CVC procedure will be performed using setting number three (#
3).
The colonoscopy protocol will be the same in both participating centres. All patients will
undergo a bowel preparation consisting in the intake of four litres of hypertonic
polyethylene glycol solution. The procedures will be performed under conscious sedation using
propofol. The caecum will be reached in white light endoscopy in all cases. Cecal intubation
will be confirmed by identification of the ileocecal valve and appendiceal orifice. Upon
extubation, 20 mg of butyl scopolamine will be given intravenously, barring any
contraindication, to reduce colonic motility and facilitate the examination of the colon.
When performing the FICE procedure, the imaging mode will be switched to CVC at the caecum
and will then be used throughout withdrawal. The endoscopist will classify the degree of
inflammation in each segment of the colon on a scale and give the Mayo Clinic score
(proctosigmoiditis - left-sided colitis - Pan Colitis). The quality of the bowel preparation
will be noted. During the extubation phase, washing of the colon and aspiration of waste will
be accomplished in an optimal way to maximise the detection capabilities of each procedure.
The biopsy protocol is meant to reflect observed mucosal abnormalities and, in the case of
conventional colonoscopy, it will be supplemented by random samples taken every 10 cm of the
colon. A standard biopsy forceps will be used (Radial Jaw 4, Boston Scientific Inc., USA). To
reduce the risk of sampling error, a minimum of two biopsies for each suspicious lesion will
be performed. The number of lesions suspect of neoplasia will be noted and targeted by each
procedure. In the case of high-resolution FICE colonoscopy, an analysis of the surface
pattern will be performed for each targeted lesion according to the pit pattern
classification. Suspicious FICE lesions will be defined as having a polyploidy, flat or
irregular mucosal structure with Kudo pit pattern III - V, unusual ulcers, strictures or
areas with increased and disrupted vascular intensity revealed by dark
coloration/discoloration and confirmed with magnification (annexe 9). In conventional
endoscopy without FICE, suspicious lesions will be defined as polypoid or irregular mucosa,
and unusual ulcers or strictures. During the conventional white light endoscopy (but not
during FICE) additional four-quadrant random biopsies will be taken every 10 cm of colon and
placed in a specimen container of formalin. Targeted biopsy samples will be sent separately
for analysis.
The histopathological evaluation will be performed twice, by two different pathologists, at
each participating centre. The pathologists were recruited according to their expertise in
digestive histology. For the purposes of this study, they will be blinded to the assessment
of the endoscopist when analysing biopsy samples. The inflammation activity level of each
specimen will be ranked into the following categories: no inflammation, mild to moderate
inflammation or severe inflammation. Dysplasia will be classified according to the new Vienna
classification 21. Lesions classified as "indefinite for neoplasia" with no differentiation
between adenoma and colitis-associated dysplasia in biopsy material will be not considered as
neoplastic. The final histopathology findings will then be compared with the endoscopic
assessment with regards to the presence of intraepithelial neoplasia and colorectal cancer.
