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Expression of E-cadherin and p53 proteins in human soft tissue sarcomas.

作者信息

Yoo Jinyoung, Park Sonya, Kang Chang Suk, Kang Seok Jin, Kim Byung Kee

机构信息

Department of Pathology, St Vincent's Hospital, Catholic University, Kyungkido, South Korea.

出版信息

Arch Pathol Lab Med. 2002 Jan;126(1):33-8. doi: 10.5858/2002-126-0033-EOECAP.

Abstract

OBJECTIVE

To investigate the expression of E-cadherin in human soft tissue sarcomas and its potential relationship to p53 alterations.

DESIGN

Tissue sections of 91 soft tissue sarcomas were analyzed by immunohistochemistry for E-cadherin and p53 proteins. Sixty-one tumors were investigated further by the application of the polymerase chain reaction technique and a direct sequence analysis procedure of exons 5 through 8 in the p53 gene.

SETTING

Tertiary-care teaching hospital.

PATIENTS

Ninety-one patients with soft tissue tumor were treated surgically. Thirteen of these patients had tumors with epithelial differentiation.

RESULTS

E-Cadherin was expressed at the cell-cell boundaries in 11 samples (12%): 9/13 (69%) with and 2/78 (3%) without histologic evidence of epithelial elements. Other sarcomas were completely negative for E-cadherin. Overexpression of p53 was detected in 30 cases (33%), 7 of which also demonstrated mutations in the p53 gene. The frequencies of p53 abnormalities in tumors with and without epithelial components were 8% and 37%, respectively. No association was established between E-cadherin immunoreactivity and p53 abnormalities (P =.13). Tumor grade strongly correlated with p53 alterations (P =.01), but not with E-cadherin expression (P =.07).

CONCLUSIONS

These data support the involvement of p53 alterations in the pathogenesis of soft tissue sarcomas. The lack of E-cadherin expression in these tumors, with the exception of lesions showing epithelial differentiation, indicates that E-cadherin is not an important factor involved in cell-cell adhesion in sarcomas. It is, however, suggested that E-cadherin may play a role in the development and/or maintenance of epithelial architecture in sarcomas, regardless of p53 status.

摘要

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