Functional Dyspepsia Clinical Trial
Official title:
Minimal Changes of Gastric Mucosal Barrier in the Pathophysiologic Mechanisms of Functional Dyspepsia
There has been recent interest into the potential role of mucosal barrier defects in the pathophysiology of functional gastrointestinal disorders (FGIDs). There has been evidence of increased intestinal permeability in patients of IBS,and abnormal tissue resistance in NERD. Although the mucosa of Functional dyspepsia (FD) patients is endoscopically and histologically "normal," it contains ultrastructural changes, activated immune cells, along with evidence of an increased release of mediators leading to gastric dysfunction. There is now consistent evidence indicating that mucosal barrier defects allow the passage of an increased load of bacteria, antigens and toxins which, in turn evoke activation of mucosal immune responses involved in the FD symptom.
Confocal laser endomicrosopy is a newly developed device which allows in vivo and real time
observation of gastrointestinal mucosa.In our pilot study we found that the contrast agent
fluorescein sodium shew differences of leakage into intercellular spaces and crypt lumen
among different patients of FD.
This study is aimed to determine if there is microscopic changes detectable in the gastric
mucosal epithelium through confocal endomicroscopy of FD patients, and to evaluate the
relationship among minimal changes(transmission electron microscopy and Confocal laser
endomicrosopy ), FD symptoms(symptom index form) , neuropeptides and immune
responses(immunohistochemistry).
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Observational Model: Case Control, Time Perspective: Prospective
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