Effect of Antireflux Therapy on the Expression of Genes in Patients With GERD

University of Rochester

Status

Terminated

Conditions

Gastroesophageal Reflux

GERD

Treatments

Drug: Prevacid Solutabs

Procedure: Antireflux surgery

Study type

Observational

Funder types

Other

Industry

Identifiers

NCT00624546

rsrb18199

RSRB18199

Details and patient eligibility

About

Although the symptomatic and epithelial (histologic and endoscopic) response to antireflux therapy are well known and extensively studied, little is known of the genetic events occurring in response to proton pump inhibitor therapy. Preliminary data from our laboratory has shown, for example, that COX-2 expression is not only elevated in patients with gastroesophageal reflux disease but also can be correlated with pathologic esophageal acid exposure on 24 hour pH monitoring. Similar studies have suggested that antireflux surgery may normalize COX-2 gene expression. In contrast studies following ablation of dysplastic Barrett's epithelium have shown persistence of genetic changes associated with altered cellular function, despite the return of the histologic appearance to normal. Several key mediators of inflammation, metaplasia (Barrett's) and neoplasia have now been well characterized and shown to be important factors in the pathogenesis of esophageal injury. It is likely that successful antireflux therapy returns altered expression of these mediators toward normal although this hypothesis remains largely unexplored. The aim of this study is to investigate gene expression of key mediators of the spectrum of esophageal mucosal injury and the response to antireflux therapy.

Hypothesis: Antireflux therapy (proton pump inhibitor and surgical fundoplication) normalizes the expression of genes known to be involved in the pathogenesis of inflammation (esophagitis), metaplasia (Barrett esophagus) and neoplasia (adenocarcinoma).

Full description

Aims: To determine the effects of antireflux therapy (pump inhibitor and surgical fundoplication) on gene expression of:

inflammation: IL-8, IFN-g, TNF-a.
intestinal metaplasia: CDX-1/2, MUC2 and Sonic hedgehog.
Neoplasia: Cox-2, VEGF, and EGFR.

Enrollment

24 patients

Sex

All

Ages

18 to 74 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

For patients with GERD

Patients referred for anti-reflux surgery
On PPI therapy for at least 6 months
Positive ambulatory pH monitoring (%time pH<4 > 4.7)
Age greater than 18 years old.
Both genders

For non-GERD controls

Negative ambulatory pH monitoring OR
Upper endoscopy performed for non-GERD symptoms.
Age greater than 18 years old.
Both genders

Exclusion criteria

Prior foregut surgery
Contra-indications for operation (poor clinical status, etc.)
Contra-indications for endoscopy and biopsy (esophageal or gastric varices, therapeutic anticoagulation with Coumadin or Heparin, etc.)
Unwillingness to participate in all of the follow-up studies
Pregnancy
Patients using medications that may interfere with PPIs pharmacokinetics (sucralfate, ketoconazole (Nizoral), ampicillin (Omnipen, Principen), digoxin (Lanoxin, Lanoxicaps), and iron (Feosol, Mol-Iron, Fergon, Femiron).
Patients using medications that may interfere with gene expression (Immunosuppressants, Aspirin, NSAIDs, Corticosteroids).
Patients with diseases that may interfere with gene expression (autoimmune diseases, diseases that course with immunosuppression).