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Literature DB >> 27699033

Effect of ARID1A/BAF250a expression on carcinogenesis and clinicopathological factors in pure-type clear cell adenocarcinoma of the ovary.

Masafumi Kato¹, Masashi Takano¹, Morikazu Miyamoto¹, Naoki Sasaki¹, Tomoko Goto¹, Ayako Suzuki¹, Junko Hirata¹, Hidenori Sasa¹, Hitoshi Tsuda², Kenichi Furuya¹.

Abstract

Frequent mutation of the ARID1A gene has been recently identified in ovarian clear-cell adenocarcinoma (CCA); however, the clinical significance of BAF250a expression encoded by the ARID1A gene remains to be determined. The aim of the present study was to assess whether BAF250a expression had an impact on the clinical features of CCA. A total of 97 cases of CCA treated at a single institution were enrolled in the present study. The tissue samples were evaluated by immunohistochemical staining. BAF250a-deficient expression was observed in 30% (29/97) of all CCA cases. Of this, 19% of non-atypical endometriosis, 26% of atypical endometriosis, 39% of endometriosis-related CCA, 5% of benign clear-cell adenofibroma (CCAF), 5% of borderline CCAF and 10% of CCAF-related CCA. BAF250a-deficient expression was significantly more frequent in endometriosis-related CCA compared with that in CCAF-related CCA (P=0.02). No significant difference was observed in the response rate of primary chemotherapy according to BAF250a expression status (P=0.48). Additionally, BAF250a expression status was not significantly correlated with progression-free and overall survival in patients with CCA. Although loss of BAF250a expression was associated with early tumorigenesis in endometriosis-related CCA, this alteration was not significantly correlated with chemosensitivity and prognoses of CCA. Further biomarker analyses, including BAF250a expression, are required to improve the prognoses of CCA.

Entities: Disease Gene Species

Keywords: ARID1A; BAF250a; clear cell adenocarcinoma; endometriosis; ovarian cancer; overall survival; progression-free survival

Year: 2016 PMID： 27699033 PMCID： PMC5038207 DOI： 10.3892/mco.2016.973

Source DB: PubMed Journal: Mol Clin Oncol ISSN： 2049-9450

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