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间充质肿瘤中的细胞核β-连环蛋白

Nuclear beta-catenin in mesenchymal tumors.

作者信息

Ng Tony L, Gown Allen M, Barry Todd S, Cheang Maggie C U, Chan Andy K W, Turbin Dmitry A, Hsu Forrest D, West Robert B, Nielsen Torsten O

机构信息

Genetic Pathology Evaluation Centre, University of British Columbia, Vancouver, British Columbia, Canada.

出版信息

Mod Pathol. 2005 Jan;18(1):68-74. doi: 10.1038/modpathol.3800272.

Abstract

Beta-catenin is a crucial part of the Wnt and E-cadherin signalling pathways, which are involved in tumorigenesis. Dysregulation of these pathways allow beta-catenin to accumulate and translocate to the nucleus, where it may activate oncogenes. Such nuclear accumulation can be detected by immunohistochemistry, which may be useful in diagnosis. Although the role of beta-catenin has been established in various types of carcinomas, relatively little is known about its status in mesenchymal tumors. A number of studies suggest that beta-catenin dysregulation is important in desmoid-type fibromatosis, as well as in synovial sarcoma. We wished to determine whether nuclear beta-catenin expression is specific to and sensitive for particular bone and soft-tissue tumors, including sporadic desmoid-type fibromatosis. We studied the nuclear expression of beta-catenin using tissue microarrays in a comprehensive range of bone and soft-tissue tumor types. A total of 549 cases were included in our panel. Nuclear immunohistochemical staining was determined to be either high level (>25% of cells), low level (0-25%) or none. High-level nuclear beta-catenin staining was seen in a very limited subset of tumor types, including desmoid-type fibromatosis (71% of cases), solitary fibrous tumor (40%), endometrial stromal sarcoma (40%) and synovial sarcoma (28%). Although occasional cases of fibrosarcoma, clear cell sarcoma and carcinosarcoma had high-level staining, no high-level nuclear beta-catenin expression was seen in any of 381 fibrohistocytic, muscular, adipocytic, chondroid or osseous tumor cases representing 42 diagnostic categories. All primary immunostain tissue microarray images are made publicly accessible in a searchable database. High-level nuclear beta-catenin staining serves as a useful diagnostic tool, as it is specific to a small subset of mesenchymal tumors.

摘要

β-连环蛋白是Wnt和E-钙黏蛋白信号通路的关键组成部分,这些信号通路参与肿瘤发生。这些信号通路的失调会使β-连环蛋白积累并转移至细胞核,在细胞核中它可能激活癌基因。这种细胞核内的积累可通过免疫组织化学检测到,这在诊断中可能有用。尽管β-连环蛋白在各种类型的癌中的作用已得到确立,但关于其在间叶性肿瘤中的状态却知之甚少。多项研究表明,β-连环蛋白失调在韧带样型纤维瘤病以及滑膜肉瘤中很重要。我们希望确定细胞核β-连环蛋白表达对于特定的骨和软组织肿瘤,包括散发性韧带样型纤维瘤病,是否具有特异性和敏感性。我们使用组织微阵列研究了一系列广泛的骨和软组织肿瘤类型中β-连环蛋白的细胞核表达。我们的样本共纳入了549例病例。细胞核免疫组织化学染色被判定为高水平(>25%的细胞)、低水平(0-25%)或无染色。在非常有限的一部分肿瘤类型中可见高水平的细胞核β-连环蛋白染色,包括韧带样型纤维瘤病(71%的病例)、孤立性纤维性肿瘤(40%)、子宫内膜间质肉瘤(40%)和滑膜肉瘤(28%)。尽管偶尔有纤维肉瘤、透明细胞肉瘤和癌肉瘤病例有高水平染色,但在代表42种诊断类别的381例纤维组织细胞性、肌肉性、脂肪性、软骨样或骨性肿瘤病例中,均未见到高水平的细胞核β-连环蛋白表达。所有原发性免疫染色组织微阵列图像都在一个可搜索的数据库中公开提供。高水平的细胞核β-连环蛋白染色是一种有用的诊断工具,因为它对一小部分间叶性肿瘤具有特异性。

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