基于生物标志物表达的综合评价SOX2是睾丸和妇科胚胎型神经外胚层肿瘤(ENT)中最敏感的生物标志物

IF 4.2 1区 医学 Q1 PATHOLOGY
Jessica F Williams, Krzysztof Glomski, Thomas M Ulbright, Krisztina Z Hanley, Kenneth A Iczkowski, Andres M Acosta, Marisa R Nucci, Esther Oliva, Michelle S Hirsch
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引用次数: 0

摘要

睾丸和妇科的胚胎型神经外胚层肿瘤(ENT,以前称为原始神经外胚层肿瘤,PNET)与小的圆形蓝细胞肿瘤(包括尤文氏肉瘤(ES))具有相同的形态学特征,但在生物学、治疗和预后方面都不同。耳鼻喉科的诊断具有挑战性,目前尚不清楚是否有可靠的生物标志物可用于确认这种诊断。本研究发现50例发生于睾丸(38例)和妇科(12例,卵巢7例/子宫5例)的ENTs,有27种生物标志物(AE1/AE3、ATRX、CD99、chromogranin-A、Cyclin D1、Fli-1、GFAP、GLUT-1、idh2 /2、INSM1、MTAP、NANOG、Nestin、neurofilament、NKX2.2、NSE、OCT3/4、OLIG2、p16、PAX6、PHOX2B、S100、SALL4、SOX2、SOX10、SOX17、synaptophysin)。评估表达程度(0,阴性,1,≤10%阳性,2,11% ~ 50%阳性,3,50%阳性)和染色强度(1,弱,2,中等,3,强),得到综合评分(CS) 0-9;CS≥4为“显著染色”。SOX2是耳鼻喉科最敏感的生物标志物,85%的肿瘤CS=9。在半数以上的ENTs中,GLUT-1、Fli-1、SALL4和Cyclin D1也显示CS≥4;然而,只有少数人的CS=9。所有其他生物标志物在不到一半的ENTs中显示CS≥4,包括突触素(38%)、GFAP(15%)、S100(15%)和嗜铬粒蛋白- a(14%)。NKX2.2、CD99和SOX17分别在7%、0%和3%的肿瘤中CS≥4。总的来说,我们发现在适当的临床病理背景下,使用SOX2、OCT3/4(排除胚胎癌)、AE1/AE3、NKX2.2、CD99和SOX17的组合可能有助于耳鼻喉科的诊断;许多其他传统的诊断生物标志物显示出有限的效用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
SOX2 Is the Most Sensitive Biomarker in Testicular and Gynecologic Embryonic-type Neuroectodermal Tumors (ENT) Based on a Comprehensive Evaluation of Biomarker Expression.

Embryonic-type neuroectodermal tumor (ENT; previously referred to as primitive neuroectodermal tumor, PNET) of the testis and gynecologic tract share morphologic features with small round blue cell tumors, including Ewing sarcoma (ES), yet are biologically, therapeutically, and prognostically distinct. The diagnosis of ENT can be challenging, and it is unclear if there are reliable biomarkers that can be used to confirm this diagnosis. This study characterized 50 ENTs arising from the testis (n=38) and gynecologic tract (n=12; 7 ovary/5 uterus) with 27 biomarkers (AE1/AE3, ATRX, CD99, chromogranin-A, Cyclin D1, Fli-1, GFAP, GLUT-1, IDH1/2, INSM1, MTAP, NANOG, Nestin, neurofilament, NKX2.2, NSE, OCT3/4, OLIG2, p16, PAX6, PHOX2B, S100, SALL4, SOX2, SOX10, SOX17, synaptophysin). Expression was evaluated for extent (0, negative; 1, ≤10% positive; 2, 11% to 50% positive; 3, >50% positive) and intensity (1, weak; 2, moderate; 3, strong) of staining to obtain a combined score (CS) of 0-9; a CS ≥4 was considered "significant staining." SOX2 was the most sensitive biomarker for ENT, as 85% of the tumors demonstrated CS=9. GLUT-1, Fli-1, SALL4, and Cyclin D1 also showed CS ≥4 in more than half of the ENTs; however, only a minority demonstrated CS=9. All other biomarkers showed CS ≥4 in fewer than half of the ENTs, including synaptophysin (38%), GFAP (15%), S100 (15%), and chromogranin-A (14%). NKX2.2, CD99, and SOX17 showed CS ≥4 in 7%, 0%, and 3% of tumors, respectively. Overall, we found that in the appropriate clinicopathologic context, utilizing a panel of SOX2, OCT3/4 (to exclude embryonal carcinoma), AE1/AE3, NKX2.2, CD99, and SOX17 could be helpful in the diagnosis of ENT; many other traditional diagnostic biomarkers show limited utility.

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来源期刊
CiteScore
10.30
自引率
5.40%
发文量
295
审稿时长
1 months
期刊介绍: The American Journal of Surgical Pathology has achieved worldwide recognition for its outstanding coverage of the state of the art in human surgical pathology. In each monthly issue, experts present original articles, review articles, detailed case reports, and special features, enhanced by superb illustrations. Coverage encompasses technical methods, diagnostic aids, and frozen-section diagnosis, in addition to detailed pathologic studies of a wide range of disease entities. Official Journal of The Arthur Purdy Stout Society of Surgical Pathologists and The Gastrointestinal Pathology Society.
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