APC; Presenting Author: WENYI XIE Corresponding Author: WENYI XIE Affiliations: the ninth hospital of Chongqing Objective: To Selleckchem PD0325901 compare the expression of COX-2 mRNA in Barrett esophagus before and after treatment, analyze the efficacy of argon plasma coagulation in combination with acid suppression in BE patients. Methods: The BE patients diagnosed with endoscopy and biopsy were randomly classified into 3 groups, group A served as control, group B treated with PPI after APC, gourp C subjected to PPI treatment.
The clinical effect was observed in the follow-up patients and endosopy examination were taken. We used quantitive real-time PCR (Taqman) to access the mRNA expression of COX-2 in Barrett esophagus before and after treatment. Total tissue RNA was extracted from Proteasome inhibitor BE. COX-2 mRNA was quantitatively analyzed by monitoring
the increase in fluorescence by the binding of SYBR green to double-stranded DNA during real-time PCR (Sequence detection system, TaqMan; Applied Biosystems, CA). The copy numbers of cDNA for COX-2 were standardized to glyceraldehyde-3-phosphate dehydrogenase from the same samples. Results: 1) All the treatment can alleviate or relieve the symptoms of BE compared to group A. There were no significant differences between them. 2) Patients of group B whose BE epithelium were eradicated and replaced with squamous epithelium. The sizes of Barrett’s esophagus didn’t change significantly in group A, C by endoscopy. 3) MCE公司 The expression of Cox-2 in groupB is similar to the level of sham-control. The expression of Cox-2 in groupC also decrease, but there was no significant differences before and after treatment. Conclusion: PPI treatment can’t eradicate BE, but they can relieve clinical symptoms and decrease the expression of Cox-2 in BE epithelium. Argon plasma coagulation combined with PPI can eradicate BE epithelium and relieve clinical symptoms and decrease the expression of Cox-2 to the normal level. It is an effective, safe and promising therapy against Barrett’s esophagus. Key Word(s): 1. Barrett’s esophagus; 2. COX-2; 3. Bcl-2; 4. APC; Presenting Author: DIANCHUN FANG Additional Authors: JUN WANG Corresponding Author: DIANCHUN FANG
Affiliations: A member of standing committee, Association of Chinese Digestive Disease Objective: To investigate the effects of bile salt exposure on expression of tight junction proteins claudin-4 in squamous epithelium of gastroesophageal reflux disease and the role of the p38 MAPK in this course. Methods: Tissue samples from 80 patients with reflux esophagitis (RE, n = 31), and Nonerosive reflux disease (NERD, n = 29) and Barrett’s esophagus (BE, n = 20) were obtained in routine upper GI endoscopy. Expression of claudin-4 in tissue samples were measured by immunohistochemical staining. Expressions of claudin-4 and p38 in esophageal squamous cells treated by bile salt were detected with reverse trancriptase polymerase chain reaction (RT-PCR) and western blot method.