Crohn Disease Clinical Trial
Official title:
Reduced Intestinal Motility in Inflammatory Crohn's Disease
Crohn's disease (CD) is becoming more common. One of the main features of this disease is
weight loss and malnutrition with symptoms such as tummy aches and bloating. These problems
have a strong negative effect on the patients' quality of life but the causes of these
problems are not well understood. Enteroendocrine cells are nutrient sensors in the bowel
that secrete special chemicals (called hormones) that control appetite and the movements all
the gut. The investigators think that this control mechanism goes wrong in Crohn's patients
and they have set off to do more research on this. Looking at the inside work of the gut has
always been difficult and at times unpleasant for patients, however recent developments in
magnetic resonance imaging (MRI) are allowing the investigators to study the workings of the
gut in greater detail and without discomfort for the patients.
Our main objective is to investigate the difference in small bowel motility between CD
patients with active ileal disease and healthy volunteers.
Background: Poor nutrition in Crohn's disease (CD) is common but poorly understood. Apart
from disease burden and repeated surgery, reduction in appetite might be an aetiological
factor.
Enteroendocrine cells (EC) are intraluminal nutrient sensors. They play a pivotal role in
orchestrating physiological functions in the gastrointestinal tract. Sensing the nutrient
content of the lumen, they secrete multiple peptides and amines that control gut secretory
and motor functions. CD patients with small bowel inflammation show increased expression in
EC peptides with exaggerated postprandial responses in anorectic EC hormones. This is
associated with symptoms of nausea and anorexia, with EC-peptide expression decreasing to
normality in remission.
There has been a longstanding interest on the effect of CD on gastric emptying and
gastrointestinal motility. Recent technological advances have allowed us to use magnetic
resonance imaging (MRI) to measure both disease activity and intestinal motility.
Reduced intestinal motility has been recently shown in CD patients with active terminal ileal
disease. A significant negative correlation is observed between terminal ileal motility and
histological, biochemical and radiological measures of disease activity. Intestinal
hypomotility may be observed in proximal unaffected segments of small bowel as well.
An increase in EC activity could potentially lead to altered appetite and symptoms of nausea
through delayed gastric emptying and most importantly delayed small bowel transit. This
mechanistic link has not been described and present findings have not been correlated to
patient symptoms. This work can potentially open a new therapeutic pathway in CD therapy.
Optimisation studies in healthy volunteers (HV) are urgently needed.
Aims & Hypothesis: In intestinal inflammation due to CD, the observed up-regulation of
fasting and postprandial EC peptides may correlate with a delayed whole gut transit
specifically small bowel transit and gastric emptying.
Experimental protocol and methods: 15 Crohn's patients and 20 Healthy volunteers will be
recruited. Standard MRI exclusion criteria will apply.
This study will have an open-label design. The subjects will be asked to fast from 2000 h.
They will be asked to fill in a questionnaire to ensure adherence to the study day
restrictions.
On the day of the scan, they will only be allowed a small glass of water on waking. They will
undergo a baseline fasting scan at 0900 hours (defined at t = -45 min time point), together
with a fasting baseline blood sample. At 0925 hours, they will be asked to eat their test
meal within a maximum time of 20 min so that at 0945 hours the subjects will undergo a first
immediate postprandial scan (defined as t = 0 min). This will be followed with data
collection (MRI, questionnaire data and blood samples) time points every 15 min for the first
60 min and every 30 min up to 270 min.
At each time point, the positioning of the subject, setup and data collection will take
~15min. After the first 60 min, at completion of data collection at each time-point, the
volunteers will be kept sitting upright in a quiet lounge next to the scanner. At each time
point, volunteers will fill a 100mm Visual Analogue Scale (VAS) symptoms questionnaire
scoring their feeling of fullness, bloating, distension, abdominal pain/discomfort and
nausea. The VAS anchors were from 'not' to 'extremely'. Participants will be given a meal at
the end of the study.
Participants will be then given a volume (750mls-1000mls) of contrast agent to drink (within
45 minutes) and a further MRI scan (time=30 minutes) will be undertaken to quantify disease
activity. Participants will be given a meal at the end of the study. This is not part of the
research protocol.
MRI scanning will be carried out supine on either a 1.5T or 3.0 T Philips Achieva MRI scanner
(Philips Healthcare, Best, The Netherlands) depending on availability. Fasting and
post-prandial plasma tests: On the morning of the test, a 10 ml fasting blood sample will be
drawn in aprotonin/EDTA tubes (BD-361017, BD Diagnostics, Oxford). Samples will be measured
every 15 min to 270 min. Samples will be centrifuged at 4000 rpm for 5 min and stored on ice.
Measurement of plasma peptides: All EC peptides (GLP-1, PYY) will be analysed through ELISA
techniques (Millipore, UK). Serum CCK will be measured by RIA (Euro Diagnostic Products,
Sweden). Total EC plasma peptide response will be presented as per individual time points and
compositely as area under the curve (AUC).
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