Crohn Disease Clinical Trial
Official title:
Significance of Ficolin 2 in the Determination of Serological Activity in Chronic Inflammatory Bowel Disease
Background Determining disease activity in IBD is sometimes difficult and, to be accurate,
requires endoscopy. The serum marker CRP has not proven sufficiently valuable as a marker
for IBD specific inflammation. As an alternative, so far fecal calprotectin appears to be
more reliable and has shown a certain value as predictive marker. Our preliminary data now
show, that the serum concentrations of ficolin-2 are significantly higher in CD patients
with a HBI >3. Ficolin-2 is a lectin and acute phase protein produced in the liver and, like
MBL, can activate the lectin pathway of complement. Unlike MBL, deficiency for ficolin-2 was
not detected in our patient cohort, nor could we find functional deficiencies for ficolin-2
(paper submitted).
Study Aims The study is aimed to substantiate the data from our pilot study which shows that
ficolin-2 is significantly increased in CD patients during inflammation. Therefore, the
study will measure ficolin-2 concentrations in a sufficiently large patient group to obtain
enough statistical power and to compare these results with the endoscopic disease score
(SES-CD) and CRP and calprotectin values. Statistical analysis of the data will show us if
ficolin-2 is a reliable and easy to obtain new marker for active inflammation in CD.
Study Design Based on a power analysis 112 CD patients and 112 UC patients need to be
analyzed. They will be recruited from Bern, Basel and Lausanne. Only patients with routine
endoscopy will be included in the study and will be scored by SES-CD. Blood samples will be
collected at the day of endoscopy. Stool sample will be collected within the same week of
endoscopy. Calprotectin and CRP concentrations will be determined by routine diagnostics,
ficolin-2 concentrations will be determined by ELISA in our laboratory. Finally, all data
will be statistically analyzed.
Background
Background Like mannan-binding lectin (MBL), ficolins are important soluble receptors for
microbial associated molecular patterns leading to the activation of the lectin pathway
complement. Ficolins are structurally related to MBL, but due to their different
carbohydrate recognition domain represent an own family of lectins (1). The single
polypeptide chains of ficolins form trimers and the trimers finally form higher order
structures (tetramers up to hexamers) which constitute the functional protein. Humans have
three ficolins: Ficolin-1 (M-ficolin), -2 (L-ficolin) and -3 (H-ficolin), whereas ficolin-2
and -3 are present in the serum, ficolin-1 is found on the surface of monocytes. Both,
ficolin-2 and -3 are produced in the liver with an additional source for ficolin-3 in the
lung. Like MBL, ficolins have to assemble with the MBL-associated serin proteases (MASPs) in
order to activate the complement pathway (1). In our study on a possible role for the
influence of the complement system in the development of CD-associated anti-Saccharomyces
cerevisiae antibodies (ASCAs), we noticed that chronic inflammatory bowel disease (CIBD)
patients, specifically Crohn's disease (CD) patients, exhibited high serum ficolin 2
concentrations.
Our research group is interested in the interaction of the innate immune system with
microorganisms of the intestinal flora, focusing on possible defects in innate immune
mechanisms. We have more than ten years experience in the field, with a special focus on
ASCA and MBL. We have been able to continuously publish our work about these theories.
Our earlier and present studies on the role of MBL and the lectin pathway of complement in
CD led to the finding of increased ficolin-2 concentration in the sera of CD patients.
Moreover, we found that CD patients with a Harvey-Bradshaw index >3 had significantly higher
ficolin 2 concentrations than those with a Harvey-Bradshaw index of ≤ 3.
Study Hypotheses
The following hypotheses are to be tested:
1. The ficolin 2 concentration is higher in Crohn's patients with active disease than in
CD patients in remission.
2. Ficolin 2 correlates with endoscopic activity.
3. Ficolin 2 correlates with calprotectin.
Objective
The findings from the first part of the study are to be confirmed in a prospective and more
detailed study with a larger patient cohort, testing our (new) working hypothesis that
ficolin 2 represents a serum marker for disease activity in CD.
Since it is currently difficult to reliably determine disease activity in CD patients using
serum and stool markers without simultaneous endoscopic examination, another specific and
easy to obtain disease marker which correlates well with disease activity would be highly
welcome. Particularly because the current standard marker, to monitor disease activity
(faecal calprotectin), is much less accepted than testing for parameters in the blood.
Therefore, the study aims at answering the question of whether ficolin 2 is present in
greater concentrations in the blood of Crohn's patients with active inflammation compared to
CD patients in remission or to ulcerative colitis (UC) patients.
Methods
For the purposes of the study, the endoscopic activity index will be recorded using the
SES-CD (simplified endoscopic score for CD) for Crohn's patients and the Mayo score for
colitis patients.
Approximately 5 ml blood will be taken to prepare serum. (5.5 ml or 4.9 ml S Monovette or
4.7 ml or 4.9 ml serum gel Monovette).
A second test tube of blood will be taken for CRP determination. In order to measure
calprotectin, the patient will be asked to provide a stool sample shortly before or shortly
after the endoscopic examination (within one week).
Serum ficolin values are measured by enzyme-linked immune sorbent assay (ELISA) in the
laboratory at the Department of Clinical Research, University of Bern; all other values are
determined in routine diagnostic laboratories.
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Observational Model: Case-Only, Time Perspective: Cross-Sectional
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