Studying the Role of IMP3 and P53 in Detection of Dysplastic Changes in Barrett's Esophagus

Authors

The Departments of Pathology* and Hepatology, Gastroenterology & Infectious Diseases**, Faculty of Medicine, Benha University

Abstract

Abstract Background: Barrett's esophagus (BE) is an acquired metaplastic lesion with unpredictable potential for esophageal adenocarcinoma (EAC). Searching for immunohistochemical markers for predicting progression in Barrett's esophagus is of increasing interest. Aim of Study: The aim of this study is to detect early dysplastic changes in patients with BE for better management of diagnosed cases. Material and Methods: This retrospective study was carried upon 28 endoscopic biopsies of BE; 6 cases of Barrett's esophagus without dysplasia, 12 cases were Barrett's esophagus with low grade dysplasia and 10 cases with high grade dys-plasia. Cases were collected from archives of Pathology Department and Early Cancer Detection Unit (ECDU), Faculty of Medicine, Benha University during the years 2015-2020. IMP3 and P53 immunohistochemichal staining were performed and evaluated for each case. Results: IMP3 was positive with high expression in 80% of high grade dysplasia cases which was a statistically signif-icant relation between IMP3 expression and grade of dysplasia. P53 was a highly sensitive marker for early dysplastic changes, reporting 100% sensitivity to low grade dysplasia. P53 was also highly specific to high grade dysplasia (100%). IMP3 was found to be highly sensitive to high grade dysplastic changes (90%). Conclusion: Combination of both markers could be helpful in detection of early dysplastic changes in Barrett's esophagus patients who are at risk of malignancy to start a strict follow-up procedures. Both markers together could be useful in detection ofhigh grade dysplasiaand rapid intervention to prevent malignant transformation.

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