A comprehensive analysis of SOX17 expression by immunohistochemistry in human epithelial tumors, with an emphasis on gynecologic tumors

Author:

Clark Beth Z1ORCID,Soong T Rinda1,Goel Kanika1,Elishaev Esther1,Zhao Chengquan1,Jones Terri E1,Jones Mirka W1,Skvarca Lauren B1,Motanagh Samaneh A1,Carter Gloria J1,Fine Jeffrey L1ORCID,Harinath Lakshmi1,Villatoro Tatiana M1,Yu Jing1ORCID,Bhargava Rohit1ORCID

Affiliation:

1. Department of Pathology, University of Pittsburgh School of Medicine, UPMC Magee-Womens Hospital , Pittsburgh, PA , US

Abstract

Abstract Objectives The objective of this study was to evaluate SOX17, a transcription factor from the Sry high-mobility group–related box superfamily, as a diagnostic marker to determine site of origin using both whole-tissue sections and tissue microarrays (TMAs). Methods SOX17 immunohistochemistry was performed on gynecologic and nongynecologic tissues (N = 1004) using whole-tissue sections and both internally constructed and commercially available TMAs. SOX17 nuclear reactivity was scored as positive or negative on the whole-tissue sections and using the semiquantitative H score method on TMAs. Results Using both whole-tissue sections and TMAs, SOX17 was positive in 94% (n = 155) of endometrial tumors and 96% (n = 242) of ovarian tumors. All breast cases (n = 241) and vulvar/cervical squamous cell carcinomas (n = 150) were negative. Among 1004 tumors from 20 sites, the only organs with positive tumors were ovary, uterus, and testis. Conclusions SOX17 is a sensitive and specific marker for gynecologic origin in the tissues tested and may be a valuable adjunct to PAX8 and other commonly used markers to confirm endometrial or ovarian origin. SOX17 expression is lower in mucinous tumors, endocervical adenocarcinoma, high-grade neuroendocrine tumors, and undifferentiated/dedifferentiated endometrial carcinoma.

Publisher

Oxford University Press (OUP)

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