首页> 外文期刊>The Journal of Pathology: Clinical Research >A COEUR cohort study of SATB2 expression and its prognostic value in ovarian endometrioid carcinoma
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A COEUR cohort study of SATB2 expression and its prognostic value in ovarian endometrioid carcinoma

机译:COEUR队列研究SATB2表达及其在卵巢子宫内膜样癌中的预后价值

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The aim of this study was to describe the expression of special AT‐rich sequence‐binding protein 2 (SATB2) in ovarian endometrioid carcinoma (EC). SATB2 is a nuclear matrix‐associated transcription factor that is associated with abnormal expression in certain cancers but has not been reported for ovarian carcinoma. SATB2 mRNA and protein expression was first assessed in a pilot cohort of 26 samples by Affymetrix microarray and by routine immunohistochemistry on a small tissue microarray. A large multicenter validation cohort representing the well‐characterized cases of 235 ovarian EC from the Canadian Ovarian Experimental Unified Resource (COEUR) was then used to validate this result and to assess the prognostic impact of SATB2 expression. SATB2 staining was scored as negative, weak, moderate, and strong intensity, and by percentage of stained cells. No SATB2 expression was observed in clear cell carcinomas but 10% ( n = 3) of the ECs in the pilot cohort showed SATB2 expression. In the validation cohort, strong expression was observed in 11% of ECs, while weak or moderate expression levels were detected in 12% of cases. Evaluation of SATB2 expression with clinicopathological parameters revealed an association with patient age and Federation International of Gynecology and Obstetrics grade but not with disease stage or postoperative residual disease. Any expression of SATB2, independent of intensity, was also associated with longer survival and improved progression‐free survival with hazard ratio (HR)?= 0.14 (95% CI 0.03–0.56) and HR?= 0.16 (95% CI 0.02–1.24) respectively. A greater beneficial effect was observed in patients with stage III/IV disease compared to patients with stage I/II disease. Furthermore, direct comparison of SATB2 with other reported prognostic biomarkers such as progesterone receptor, CDX2 and β‐catenin within this cohort showed that SATB2 had the strongest association with survival. Given the current lack of accurate prognostic factors for these patients, SATB2 has promising clinical utility and warrants further study.
机译:这项研究的目的是描述特殊的富含AT的序列结合蛋白2(SATB2)在卵巢子宫内膜样癌(EC)中的表达。 SATB2是一种与核基质相关的转录因子,在某些癌症中与异常表达有关,但尚未报道卵巢癌。首先通过Affymetrix微阵列和小型组织微阵列上的常规免疫组织化学方法在26个样本的试验队列中评估了SATB2 mRNA和蛋白的表达。然后,使用一个大型多中心验证队列来代表来自加拿大卵巢实验统一资源(COEUR)的235个卵巢EC的典型病例,以验证该结果并评估SATB2表达的预后影响。 SATB2染色按染色细胞的百分比分为阴性,弱,中度和强强度。在透明细胞癌中未观察到SATB2表达,但在试验队列中有10%(n = 3)的EC显示出SATB2表达。在验证队列中,在11%的EC中观察到了强表达,而在12%的病例中检测到了弱或中等表达水平。通过临床病理参数评估SATB2表达,发现患者年龄与联合会国际妇产科等级相关,但与疾病阶段或术后残留疾病无关。无论强度如何,SATB2的任何表达都与更长的生存期和更好的无进展生存期相关,风险比(HR)?= 0.14(95%CI 0.03–0.56)和HR?= 0.16(95%CI 0.02–1.24) ) 分别。与患有I / II期疾病的患者相比,在III / IV期疾病的患者中观察到更大的有益作用。此外,该人群中SATB2与其他已报道的预后生物标志物如孕酮受体,CDX2和β-catenin的直接比较表明,SATB2与生存率的关联最强。鉴于目前对于这些患者缺乏准确的预后因素,SATB2具有广阔的临床应用前景,值得进一步研究。

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