Inflammatory Bowel Disease Clinical Trial
Official title:
Characterization of Interactions Between Immune Cells of Intestinal Mucosa or Peripheral Blood With the Extracellular Matrix in IBD
The purpose of this study is to examine the effects of different environmental factors on immune cells in patients with IBD.
Background: Inflammatory bowel diseases, comprised of Crohn's Disease (CD) and ulcerative
colitis (UC) are idiopathic disorders caused due to immunological, genetic, and
environmental factors. These disorders are fairly common (in the US, there are 11 cases of
CD and 7 cases of UC for every 100,000 people). The frequency of IBD, especially CD, are
constantly rising (1). Clinical symptoms include diarrhea, rectal bleeding, abdominal pain,
intestinal obstructions, and fistulas in CD. There are also systemic manifestations such as
fever, weight loss, and anemia. The current hypothesis of IBD pathogenesis is an aberrant,
ongoing, uncontrolled inflammatory response of the intestine, caused by commensal
microbiota. The inflammatory response in IBD is mediated by T cells; in CD the pathologic
lymphocytes are CD4 cells of Th1 type, while UC is considered an atypical Th2 response (2).
CD4 T cells have a major role in initiation of inflammatory response in the gut, as well as
a role in propagation and control of the inflammation.
Chemokines are low-molecular weight cytokines with chemoattractant capacity, and have a role
in many inflammatory disorders. The chemokine CXCL12 is considered to be constitutively
expressed (3). Our group found increased expression of CXCL12 in IBD (REF?). This finding
suggests that CXCL12 might have a role in inflammatory processes of the gut.
Understanding phenotypical and functional differences of lymphocytes in mucosal homeostasis
and IBD, elucidation of factors causing these differences, and recognition of causes for
increased CXCL12 expression, will enable to increase knowledge of IBD; as well as lead to
development of future therapeutic interventions in IBD.
Research Goals: To examine the effects of different environmental factors (cytokines,
chemokines, extracellular matrix moieties) on immune cells from peripheral or intestinal
source (in homeostasis or IBD) in terms of phenotypical and functional parameters.
Methods: 15 ml peripheral blood will be obtained from all participants. T lymphocytes will
be isolated for the different experiments. Methods will include: Migration towards
chemokines using the Transwell assay, proliferation will be assessed by either BrdU or
thymidine incorporation, cytokine secretion will be determined using ELISA, phenotypical
characterization will be done using flow cytometry and adhesion assays.
Ages: Adults and children aged 10-80. Research group: Approximately 40 patients (adults and
children) suffering from IBD will be enrolled.
Control group: Approximately 100 controls will be enrolled in the research.
;
Observational Model: Case-Only, Time Perspective: Cross-Sectional
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