Syndecan-1 and E-cadherin expression in differentiated type of early gastric cancer

doi:10.3748/wjg.v11.i19.2975

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May 21, 2005 (publication date) through Apr 25, 2024

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World Journal of Gastroenterology

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1007-9327

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Baishideng Publishing Group Inc, 7041 Koll Center Parkway, Suite 160, Pleasanton, CA 94566, USA

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World J Gastroenterol. May 21, 2005; 11(19): 2975-2980
Published online May 21, 2005. doi: 10.3748/wjg.v11.i19.2975

Syndecan-1 and E-cadherin expression in differentiated type of early gastric cancer

Mei-Fang Huang, You-Qing Zhu, Zhi-Fen Chen, Jun Xiao, Xin Huang, Yong-Yan Xiong, Gui-Fang Yang

Mei-Fang Huang, You-Qing Zhu, Zhi-Fen Chen, Jun Xiao, Xin Huang, Department of Digestive Disease, Zhongnan Hospital of Wuhan University, Wuhan 430071, Hubei Province, China

Yong-Yan Xiong, Gui-Fang Yang, Department of Pathology, Zhongnan Hospital of Wuhan University, Wuhan 430071, Hubei Province, China

Author contributions: All authors contributed equally to the work.

Supported by the Medical Science Research Foundation of Hubei Province, No. 101130780

Correspondence to: You-Qing Zhu, Department of Digestive Disease, Zhongnan Hospital of Wuhan University, Wuhan 430071, Hubei Province, China. uqing-zhu@sina.com

Telephone: +86-27-67813275 Fax: +86-27-87307622

Received: July 12, 2004
Revised: July 13, 2004
Accepted: November 4, 2004
Published online: May 21, 2005

Abstract

AIM: To elucidate the role and alterations of syndecan-1 and E-cadherin expression in different cellular phenotypes of differentiated-type gastric cancers (DGCs).

METHODS: A total of 120 DGCs at an early stage, and their adjacent mucosa, were studied both by immunohis-tochemistry. Syndecan-1 and E-cadherin were assessed by immunohistochemical staining with anti-syndecan-1 and anti-E-cadherin antibodies, respectively. Based on immunohistochemistry, DGCs and their surrounding mucosa were divided into four types: gastric type (G-type), ordinary type (O-type), complete-intestinal type (CI-type), and null type (N-type).

RESULTS: Syndecan-1 expression was significantly lower in G-type cancers (29.4%) than in O-type (79.6%) and CI-type cancers (90%) (P<0.05, respectively), but E-cadherin did not show this result. In addition, syndecan-1 expression was significantly reduced in DGCs comprised partly of poorly differentiated adenocarcinoma or signet-ring cell carcinoma, compared to DGCs demonstrating papillary and/or tubular adenocarcinoma (P<0.05). G-type intestinal metaplasia (IM) surrounding the tumors was observed in 23.8% of G-type, 4.9% of O-type, and 6.7% of CI-type cancers (P<0.05; G-type vs O-type). Reduction of syndecan-1 expression was significant in G-type IM (25%) compared to non-G-type IM (75%; P<0.05).

CONCLUSION: Loss of syndecan-1 plays a role in the growth of G-type cancers of DGCs at an early stage, and the reduction of syndecan-1 expression in IM surrounding the tumors may influence the growth of G-type cancer.

Keywords: Gastric cancer, Cellular phenotype, Syndecan-1