Undifferentiated Pleomorphic Sarcoma of Soft Tissue with Multinucleated Giant Cells with Osteogenic Phenotypes: A Mimicker of Malignant Giant Cell Tumor of Soft Tissue

IF 0.3 4区 医学 Q4 ENGINEERING, BIOMEDICAL Journal of Hard Tissue Biology Pub Date : 2021-01-01 DOI:10.2485/jhtb.30.309
S. Matsuoka, H. Hasegawa, Sachie Koike, Tsutomu Koyama, T. Takeda, K. Miura, T. Eguchi, K. Hamanaka, M. Kito, J. Takahashi, Toshirou Fukushima, T. Koizumi, K. Shimizu, T. Uehara
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Abstract

: This study aimed to summarize the clinicopathological findings and assess the immunophenotypes for undifferen tiated pleomorphic sarcoma of soft tissue with multinucleated giant cells (UPS-ST-MGCs). We retrospectively identified five cases of UPS-ST-MGCs between 2010 and 2020, and evaluate histological and immunohistochemical findings using osteogenic markers, which were receptor activator of nuclear factor-kappa B ligand (RANKL), runt-related transcription factor 2 (RUNX2), and special AT-rich sequence-binding protein 2 (SATB2). Cases were divided into two types, based on the distribution of multinucleated giant cells (MGCs), as diffusely (MGCs diffuse type) or focally scattering (MGCs focal type). One out of five cases was classified as MGCs diffuse type and comprised relatively monotonous proliferation of atyp ical spindle cells widely expressing RANKL, RUNX2, and SATB2. This case showed aggressive clinicopathological features, such as a rapidly growing tumor with a high maximum standardized uptake value, high Ki-67 labeling index, and early postoperative recurrence, which can be called malignant giant cell tumor (GCT-ST). Conversely, the other four cases of the MGCs focal type were focally positive for RANKL, and negative for RUNX2 and STAB2, which appeared to be consistent with conventional features of undifferentiated pleomorphic sarcoma of soft tissue. Our results indicate that malignant GCT-ST can be included in UPS-ST-MGCs. Therefore, it is important to note its aggressive malignant characteristics and osteogenic differentiation. Osteogenic immunohistochemical examinations should be considered for UPS-ST-MGCs to con firm an accurate diagnosis and provide appropriate treatment.
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具有成骨表型的多核巨细胞的软组织未分化多形性肉瘤:软组织恶性巨细胞瘤的模拟物
本研究旨在总结多核巨细胞软组织未分化多形性肉瘤(UPS-ST-MGCs)的临床病理表现并评估其免疫表型。我们回顾性分析了2010年至2020年期间的5例UPS-ST-MGCs,并使用成骨标志物(核因子- κ B配体受体激活剂(RANKL)、矮子相关转录因子2 (RUNX2)和特殊的富含at的序列结合蛋白2 (SATB2))评估组织学和免疫组织化学结果。根据多核巨细胞(MGCs)的分布,将病例分为弥漫性(MGCs弥漫性)和局灶性(MGCs局灶性)两种类型。1 / 5的病例被归类为MGCs弥漫型,由广泛表达RANKL、RUNX2和SATB2的非典型梭形细胞组成的相对单调的增殖。该病例具有侵袭性的临床病理特征,肿瘤生长迅速,最大标准化摄取值高,Ki-67标记指数高,术后早期复发,可称为恶性巨细胞瘤(GCT-ST)。相反,其他4例MGCs局灶型RANKL局灶阳性,RUNX2和STAB2局灶阴性,这似乎与软组织未分化多形性肉瘤的常规特征一致。我们的结果表明,恶性GCT-ST可以包括在UPS-ST-MGCs中。因此,注意其侵袭性恶性特征和成骨分化是很重要的。对于UPS-ST-MGCs应考虑成骨免疫组化检查,以确定准确的诊断并提供适当的治疗。
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来源期刊
Journal of Hard Tissue Biology
Journal of Hard Tissue Biology ENGINEERING, BIOMEDICAL-
CiteScore
0.90
自引率
0.00%
发文量
28
审稿时长
6-12 weeks
期刊介绍: Information not localized
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