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[双表型鼻窦肉瘤的临床病理及分子特征]

[Clinicopathological and molecular features of biphenotypic sinonasal sarcoma].

作者信息

Wu N, Wang X, Cheng K, Wei X, Zhang R S, Lu Z F, Rao Q

机构信息

Department of Pathology, Nanjing Jinling Hospital, Nanjing University School of Medicine, Nanjing 210002, China.

出版信息

Zhonghua Bing Li Xue Za Zhi. 2020 Dec 8;49(12):1261-1266. doi: 10.3760/cma.j.cn112151-20200313-00200.

Abstract

To study the clinicopathologic features, immunophenotype, molecular genetics and differential diagnosis of biphenotypic sinonasal sarcoma (BSNS), and to evaluate the role of PAX3 and PAX8 immunohistochemical (IHC) antibodies in the diagnosis of BSNS. Nasal sinus spindle cell tumors surgically treated at the Jinling Hospital from 2000 to 2019 were collected, including three cases of BSNS, 10 cases of acinar rhabdomyosarcoma, eight cases of schwannoma, five cases of hemangiopericytoma, three cases of fibrosarcoma, and one case of triton tumor. The cases were evaluated by histology, IHC by EnVision for PAX3 and PAX 8 (including PAX8 murine monoclonal antibody, clone number OTI6H8, hereinafter referred to as PAX8-OTI6H8 antibody; PAX8 rabbit monoclonal antibody, clone number EP298, hereinafter referred to as PAX8-EP298 antibody) molecular genetic tests. All three BSNS patients were elderly women with clinical manifestations of nasal congestion and bleeding. Imaging showed a soft tissue density shadow of the nasal cavity and sinuses with bone destruction. The boundaries of tumors which were covered with ciliated columnar epithelium were unclear, and mucosal invasion and squamous metaplasia could be seen. Tumor cells were spindle-shaped, arranged in a bundle-like, braided arrangement, with little cellular atypia and occasional atypical mitotic figures. The tumoral interstitial vessels were mostly thin-walled, some showing staghorn-like changes. There was focal striated muscle differentiation in two cases, and bone invasion was seen in two cases. IHC staining showed that all three cases of BSNS expressed PAX3 and PAX8-OTI6H8, but not PAX8-EP298. All eight cases of schwannoma, five cases of hemangiopericytoma, and one case of triton tumor did not express PAX3, PAX8-OTI6H8 or PAX8-EP298. Eight of the ten cases of alveolar rhabdomyosarcoma expressed PAX3 and PAX8-OTI6H8, but not PAX8-EP298. Three cases of fibrosarcoma showed weak PAX3 and PAX8-OTI6H8 expression, but there was no PAX8-EP298 expression. FISH detection showed that PAX3 break apart in the tumor cells from all three patients (four specimens). BSNS is a distinct sinonasal low grade malignancy with dual differentiation which could be readily confused with a variety of spindle cell tumors encountered in the sinonasal cavity. The molecular genetics of PAX3 gene break is the gold standard for diagnosis of this tumor. IHC marker monoclonal PAX3 is 100% expressed in BSNS, while the specificity is limited. PAX8-OTI6H8 is also expressed in BSNS due to the cross reaction with PAX3 antibody, while PAX8-EP298 is all negative for these tumors.

摘要

研究双表型鼻窦肉瘤(BSNS)的临床病理特征、免疫表型、分子遗传学及鉴别诊断,并评估PAX3和PAX8免疫组化(IHC)抗体在BSNS诊断中的作用。收集2000年至2019年在金陵医院手术治疗的鼻窦梭形细胞肿瘤,包括3例BSNS、10例腺泡状横纹肌肉瘤、8例神经鞘瘤、5例血管外皮细胞瘤、3例纤维肉瘤和1例蝾螈瘤。通过组织学、针对PAX3和PAX8的EnVision IHC(包括PAX8鼠单克隆抗体,克隆号OTI6H8,以下简称PAX8 - OTI6H8抗体;PAX8兔单克隆抗体,克隆号EP298,以下简称PAX8 - EP298抗体)及分子遗传学检测对病例进行评估。所有3例BSNS患者均为老年女性,临床表现为鼻塞和鼻出血。影像学显示鼻腔和鼻窦软组织密度影伴骨质破坏。肿瘤边界不清,表面覆有纤毛柱状上皮,可见黏膜侵犯和鳞状化生。肿瘤细胞呈梭形,呈束状、编织状排列,细胞异型性小,偶见非典型有丝分裂象。肿瘤间质血管大多壁薄,部分呈鹿角状改变。2例有局灶性横纹肌分化,2例可见骨质侵犯。IHC染色显示,3例BSNS均表达PAX3和PAX8 - OTI6H8,但不表达PAX8 - EP298。所有8例神经鞘瘤、5例血管外皮细胞瘤和1例蝾螈瘤均不表达PAX3、PAX8 - OTI6H8或PAX8 - EP298。10例腺泡状横纹肌肉瘤中的8例表达PAX3和PAX8 - OTI6H8,但不表达PAX8 - EP298。3例纤维肉瘤PAX3和PAX8 - OTI6H8呈弱表达,但无PAX8 - EP298表达。FISH检测显示,所有3例患者(4份标本)的肿瘤细胞中PAX3均发生断裂。BSNS是一种独特的具有双分化的鼻窦低度恶性肿瘤,易与鼻窦腔中遇到的多种梭形细胞肿瘤混淆。PAX3基因断裂的分子遗传学是诊断该肿瘤的金标准。IHC标志物单克隆PAX3在BSNS中100%表达,但其特异性有限。由于与PAX3抗体的交叉反应,PAX8 - OTI6H8在BSNS中也有表达,而PAX8 - EP298在这些肿瘤中均为阴性。

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