Extra-abdominal and intra-abdominal FET::CREM fusion mesenchymal neoplasms: comparative clinicopathological study of 9 new cases further supporting a distinct potentially aggressive sarcoma and report of novel sites.

IF 3.4 3区 医学 Q1 PATHOLOGY
Abbas Agaimy, Morgan Blakely, Gerben E Breimer, Annett Hölsken, Sjors A Koppes, Norbert Meidenbauer, Johannes A Rijken, Arno Schad, Adrian G Simon, Robert Stoehr, Justin A Bishop, Nasir Ud Din
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引用次数: 0

Abstract

With the wide use of RNA sequencing technologies, the family of FET::CREB fusion mesenchymal neoplasms has expanded rapidly to include potentially aggressive neoplasms, not fitting any well established WHO entity. Recently, a group of intra-abdominal FET(EWSR1/FUS)::CREB(CREM/ATF1) fused unclassified neoplasms has been reported followed by recent recognition of an analogous extra-abdominal category of unclassified neoplasms carrying EWSR1::ATF1 fusions. We describe 9 additional tumors (5 extra-abdominal and 4 abdominal) carrying an EWSR1::CREM (n = 8) and FUS::CREM (n = 1) fusion. Patients were 7 females and 2 males aged 10 to 75 years (median, 34). Extra-abdominal tumors originated in the head and neck (2 sinonasal, 1 orbital) and soft tissues (1 gluteal, 1 inguinal). Abdominal tumors involved stomach (2), mesentery (1), and kidney (1). Tumor size ranged from 3.5 to 11 cm (median, 6). Treatment was radical surgery with (5) or without (2) neo/adjuvant radio/chemotherapy. Extended follow-up of 5 patients (21-52 months; median, 24) showed an aggressive course in two (40%); one died of disseminated metastases 52 months after several intensified chemotherapy regimens, and one was alive with progressive abdominal disease at 21 months. The immunophenotype of the two subcohorts was significantly overlapping with variable expression of EMA (7 of 8), keratin AE1/AE3 (5 of 9), CD99 (4 of 7), MUC4 (2 of 8), ALK (3 of 8), synaptophysin (3 of 9), chromogranin (1 of 8), CD34 (3 of 6), CD30 (1 of 6), PAX8 (1 of 7), and inhibin (1 of 7), but no reactivity with desmin (0 of 8), S100 (0 of 8), and SOX10 (0 of 8). This series further solidifies the notion that FET::CREB fusions are not limited to the triad of angiomatoid fibrous histiocytoma, clear cell sarcoma, and malignant gastrointestinal neuroectodermal tumor, but characterize an emerging family of potentially aggressive neoplasms occurring at both intra- and extra-abdominal sites. These tumors underscore the promiscuity of the FET::CREB fusions and highlight the pivotal role of phenotype-oriented classification of these neoplasms that share the same genotype, still featuring significant biological and behavioral distinctness.

Abstract Image

腹腔外和腹腔内 FET::CREM 融合间充质肿瘤:9 例新病例的临床病理比较研究进一步证实了一种独特的潜在侵袭性肉瘤,并报告了新的发病部位。
随着 RNA 测序技术的广泛应用,FET::CREB 融合间充质肿瘤家族迅速扩大,其中包括潜在的侵袭性肿瘤,但这些肿瘤并不符合任何已确立的 WHO 实体。最近,一组腹腔内 FET(EWSR1/FUS)::CREB(CREM/ATF1)融合的未分类肿瘤被报道出来,紧接着最近又发现了一类类似的腹腔外携带 EWSR1::ATF1 融合的未分类肿瘤。我们描述了另外 9 例携带 EWSR1::CREM(n = 8)和 FUS::CREM(n = 1)融合的肿瘤(5 例腹腔外肿瘤和 4 例腹腔肿瘤)。患者中有 7 名女性和 2 名男性,年龄在 10 至 75 岁之间(中位数为 34 岁)。腹外肿瘤起源于头颈部(2 例鼻窦,1 例眼眶)和软组织(1 例臀部,1 例腹股沟)。腹部肿瘤涉及胃(2 例)、肠系膜(1 例)和肾(1 例)。肿瘤大小从 3.5 厘米到 11 厘米不等(中位数为 6 厘米)。治疗方法为根治性手术加(5例)或不加(2例)新辅助放化疗。对5名患者的长期随访(21-52个月;中位24个月)显示,2名患者(40%)的病程具有侵袭性;1名患者在数次强化化疗后52个月死于扩散转移,1名患者在21个月时因腹部疾病进展而存活。这两个亚群的免疫表型明显重叠,EMA(8 例中的 7 例)、角蛋白 AE1/AE3 (9 例中的 5 例)、CD99(7 例中的 4 例)、MUC4(8 例中的 2 例)、ALK(8 例中的 3 例)、突触素(8 例中的 3 例)、MUC4(8 例中的 2 例)、ALK(8 例中的 3 例)、CD99(7 例中的 4 例)、MUC4(8 例中的 2 例)、突触素(8 例中的 3 例)的表达各不相同、突触素(9 个中的 3 个)、嗜铬粒蛋白(8 个中的 1 个)、CD34(6 个中的 3 个)、CD30(6 个中的 1 个)、PAX8(7 个中的 1 个)和抑制素(7 个中的 1 个),但与 desmin(8 个中的 0 个)、S100(8 个中的 0 个)和 SOX10(8 个中的 0 个)没有反应。这一系列研究进一步证实,FET::CREB 融合并不局限于血管瘤样纤维组织细胞瘤、透明细胞肉瘤和恶性胃肠道神经外胚层瘤这三种肿瘤,而是一种新出现的发生在腹腔内和腹腔外的潜在侵袭性肿瘤。这些肿瘤凸显了 FET::CREB 融合的杂合性,并强调了以表型为导向对这些具有相同基因型、但在生物学和行为学上仍有显著区别的肿瘤进行分类的关键作用。
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来源期刊
Virchows Archiv
Virchows Archiv 医学-病理学
CiteScore
7.40
自引率
2.90%
发文量
204
审稿时长
4-8 weeks
期刊介绍: Manuscripts of original studies reinforcing the evidence base of modern diagnostic pathology, using immunocytochemical, molecular and ultrastructural techniques, will be welcomed. In addition, papers on critical evaluation of diagnostic criteria but also broadsheets and guidelines with a solid evidence base will be considered. Consideration will also be given to reports of work in other fields relevant to the understanding of human pathology as well as manuscripts on the application of new methods and techniques in pathology. Submission of purely experimental articles is discouraged but manuscripts on experimental work applicable to diagnostic pathology are welcomed. Biomarker studies are welcomed but need to abide by strict rules (e.g. REMARK) of adequate sample size and relevant marker choice. Single marker studies on limited patient series without validated application will as a rule not be considered. Case reports will only be considered when they provide substantial new information with an impact on understanding disease or diagnostic practice.
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