Estrogen receptor beta expression in colitis‐associated carcinoma in comparison with sporadic colonic tumor: An immunohistochemical study

Author:

Matsuno Takahisa1ORCID,Mikami Tetuo2,Hayashi Hiroyuki3,Funahashi Kimihiko4,Okazumi Shinichi5,Hiruta Nobuyuki6,Shibuya Kazutoshi7,Igarashi Yoshinori1

Affiliation:

1. Division of Gastroenterology and Hepatology, Department of Internal Medicine Toho University Omori Medical Center Tokyo Japan

2. Department of Pathology Toho University School of Medicine Tokyo Japan

3. Department of Pathology Yokohama Municipal Citizen's Hospital Yokohama Japan

4. Department of Surgery Toho University School of Medicine Tokyo Japan

5. Department of Surgery Toho University Sakura Medical Center Sakura Japan

6. Department of Surgical Pathology Toho University Sakura Medical Center Sakura Japan

7. Department of Surgical Pathology Toho University School of Medicine Tokyo Japan

Abstract

AbstractBackground and AimThe rate of ulcerative colitis (UC)‐related colorectal cancer (colitis‐associated carcinoma) is increasing. Estrogen receptor (ER) beta expression has been studied separately in patients with sporadic colorectal cancer and those with colitis‐associated carcinoma. However, no study has compared the expression in both of these cancer types. The present study aimed to evaluate the relationship between colitis‐associated carcinoma and ERs and assess whether the expression of ER beta influences cell proliferation.MethodsThis study included 45 surgically operated colitis‐associated carcinomas, 43 high‐grade dysplasias, 34 low‐grade dysplasias, 36 sporadic colorectal cancers, 44 high‐grade adenomas, and 34 low‐grade adenomas. ER beta expression was evaluated with immunohistochemistry.ResultsColitis‐associated carcinoma showed significantly lower ER beta immunoexpression than sporadic colorectal lesions and high‐ and low‐grade dysplasia. In seven colitis‐associated carcinoma harboring both intensity score 3 (strong immunoexpression) and score 1 (weak immunoexpression) areas, the correlation among ER beta intensity, Ki‐67, and p21 labeling index was assessed; an area with an ER beta intensity score of 3 showed a higher Ki‐67 labeling index than that with score 1. In four out of the seven lesions, p21 labeling index was higher in the area of ER beta score 1 than in that of ER beta score 3.ConclusionsThe data suggest that ER beta expression is an accelerating factor in colorectal tumors. This association may be lower in colitis‐associated carcinoma than in sporadic colorectal cancer.

Publisher

Wiley

Subject

Gastroenterology,Hepatology

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