YAP1::KMT2A-Rearranged Sarcoma: Report of a New Case With Unusual Morphology and Immunohistochemical Features

IF 2.8 2区医学 Q2 GENETICS & HEREDITY

Genes, Chromosomes & Cancer Pub Date : 2025-07-11 DOI:10.1002/gcc.70059

Caterina Fumagalli, Ruth Orellana, Sílvia Bagué, Malena Ferré, Allan Gonzalez, Lluis Catasús, Jaume Llauger, Ana Peiró, Paul Zamora Alarcón, Katarina Majercakova, Raúl Terés, Marie Karanian-Philippe, Franck Tirode, Cristina R. Antonescu

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引用次数: 0

Abstract

Recurrent KMT2A and YAP1 related fusions have recently been reported in various mesenchymal neoplasms of different histogenesis. First, YAP1::KMT2A fusions have been described in a subset of MUC4-negative sclerosing epithelioid fibrosarcomas (SEF), while VIM::KMT2A fusions in a handful of cases associated with an undifferentiated spindle cell phenotype lacking stromal hyalinization. On the other hand, YAP1 gene rearrangements have been reported in a wide spectrum of sarcomas, including vascular neoplasms such as epithelioid hemangioendothelioma (EHE). Despite these molecular advances, occasional challenges in classification may occur even if the pathognomonic fusion is identified. In this study, we report such a case of a soft tissue sarcoma displaying an unusual morphology and immunoprofile, which remained unclassified even after a YAP1::KMT2A fusion was detected. The lesion occurred in the left leg of a 65-year-old female and microscopically closely resembled a SEF, with epithelioid morphology organized in cords, nests, and sheets in a heavy hyalinized background. Focally, the cells showed cytoplasmic vacuoles with eosinophilic material, reminiscent of the “blisters cells” seen in EHE. Moreover, by immunohistochemistry (IHC), the tumor showed diffuse reactivity for vascular markers, including ERG, CD31, CD34, and D2-40, as well as for TFE3, while being negative for MUC4, CAMTA1, smooth-muscle actin, desmin, S100 and keratins. Targeted RNA sequencing revealed a YAP1::KMT2A fusion. Based on this molecular result and the conflicting morphologic and IHC findings, a definitive distinction between a MUC4-negative SEF and an EHE could not been established. To further subclassify the lesion, subsequent clustering analysis using RNAseq signature was performed against a vast group of sarcoma types on the same array. Results showed that the tumor was in close proximity to the SEF group, admixed together with the other YAP1::KMT2A MUC4 negative SEF sarcomas. This case is highly instructive, as it shows another application of RNA sequencing in clinical practice when discordant or uncertain results between pathologic findings and fusion type may occur. Indeed, RNAseq signature could help, in this context, to better classify the tumor as a YAP1::KMT2A sarcoma instead of a vascular tumor. Larger series are needed to evaluate the pathogenesis of these tumors and the relevance of vascular markers expression.

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YAP1:: kmt2a重排肉瘤：新病例报告，具有异常的形态和免疫组织化学特征

KMT2A和YAP1相关的复发融合最近在各种不同组织发生的间质肿瘤中被报道。首先，YAP1::KMT2A融合在muc4阴性硬化上皮样纤维肉瘤（SEF）的一个亚群中被描述，而VIM::KMT2A融合在少数与未分化梭形细胞表型缺乏间质透明化相关的病例中被描述。另一方面，YAP1基因重排已在广泛的肉瘤中被报道，包括血管肿瘤，如上皮样血管内皮瘤（EHE）。尽管有这些分子上的进步，但即使确定了病型融合，分类上偶尔也会出现挑战。在本研究中，我们报告了一例软组织肉瘤，表现出异常的形态和免疫谱，即使在检测到YAP1::KMT2A融合后仍未分类。病变发生在一名65岁女性的左腿，显微镜下与SEF非常相似，在重透明背景下，上皮样形态呈索状、巢状和片状。局部可见嗜酸性物质的细胞质空泡，与EHE中所见的“水泡细胞”相似。此外，通过免疫组化（IHC），肿瘤对血管标志物（包括ERG、CD31、CD34和D2-40）以及TFE3表现出弥漫性反应性，而MUC4、CAMTA1、平滑肌肌动蛋白、desmin、S100和角蛋白均呈阴性。靶向RNA测序显示YAP1::KMT2A融合。基于这一分子结果以及相互矛盾的形态学和免疫组化结果，muc4阴性SEF和EHE之间的明确区别无法确定。为了进一步对病变进行亚分类，随后使用RNAseq特征对同一阵列上的大量肉瘤类型进行聚类分析。结果表明，该肿瘤与其他YAP1::KMT2A MUC4阴性SEF肉瘤混在一起，与SEF组接近。本病例具有很高的指导意义，因为它显示了RNA测序在临床实践中的另一种应用，当病理结果与融合类型之间可能出现不一致或不确定的结果时。事实上，在这种情况下，RNAseq标记可以帮助更好地将肿瘤分类为YAP1::KMT2A肉瘤而不是血管肿瘤。需要更大的系列来评估这些肿瘤的发病机制和血管标志物表达的相关性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Genes, Chromosomes & Cancer 医学-遗传学

CiteScore

7.00

自引率

8.10%

发文量

审稿时长

4-8 weeks

期刊介绍： Genes, Chromosomes & Cancer will offer rapid publication of original full-length research articles, perspectives, reviews and letters to the editors on genetic analysis as related to the study of neoplasia. The main scope of the journal is to communicate new insights into the etiology and/or pathogenesis of neoplasia, as well as molecular and cellular findings of relevance for the management of cancer patients. While preference will be given to research utilizing analytical and functional approaches, descriptive studies and case reports will also be welcomed when they offer insights regarding basic biological mechanisms or the clinical management of neoplastic disorders.