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骨外骨肉瘤中骨钙素和骨连接蛋白免疫反应性:28例研究

Osteocalcin and osteonectin immunoreactivity in extraskeletal osteosarcoma: a study of 28 cases.

作者信息

Fanburg-Smith J C, Bratthauer G L, Miettinen M

机构信息

Soft Tissue Pathology Department, Armed Forces Institute of Pathology, Washington, DC 20306-6000, USA.

出版信息

Hum Pathol. 1999 Jan;30(1):32-8. doi: 10.1016/s0046-8177(99)90297-6.

Abstract

Extraskeletal osteosarcoma (EOSA), a rare malignant soft tissue tumor, is by definition unattached to the skeleton and composed of malignant cells of osteoblastic phenotype which produce osseous matrix (ie, neoplastic bone). Because of its location, it can mimic other soft tissue tumors, and its matrix can be mistaken for hyalinized collagen. Antiosteocalcin (OC) and antiosteonectin (ON), antibodies against two abundant human bone proteins, are explored in the diagnosis of EOSA. Twenty-eight cases coded as EOSA (n=24) or probable EOSA (n = 4) were identified from the Soft Tissue Registry of the Armed Forces Institute of Pathology (Washington DC). All cases had paraffin blocks available for immunohistochemistry. OC and ON (Biodesign International, Kennebunk, ME, clones OC1 and OST1) immunostaining for tumor cells and matrix was graded on a four-tiered grading system: 1 = focal (< 50%) weak staining; 2 = focal strong staining; 3 = diffuse (> or = 50%) weak staining; and 4 = diffuse strong staining. Patient ages ranged from 9 to 80 years, with a mean age of 57 years. There were 9 female patients and 19 male patients. The tumor sizes ranged from 1.5 to 15 centimeters, with a mean size of 5.8 centimeters. Locations included the lower extremity (n=14), trunk (n=9), upper extremity (n=4), and head and neck (n=1). Subtypes included 12 osteoblastic, 4 fibroblastic, 2 chondroblastic, 2 well differentiated, 1 telangiectatic, 1 small cell, and 6 giant cell rich EOSAs; the latter resembled giant cell rich malignant fibrous histiocytomas with neoplastic bone formation. All tumors had both neoplastic cells and bony tumor matrix to evaluate. OC was 82% sensitive for EOSA neoplastic cells (1 to 4+), with immunostaining of neoplastic cells away from bone in 91% of cases, and 75% for bony tumor matrix (2 to 4+). ON was 93% sensitive for EOSA neoplastic cells (2 to 4+), yet only 39% for bony tumor matrix (1 to 4+). In 100% giant cell rich EOSA, neoplastic cells were positive for OC and ON (2 to 4+). OC showed 100% specificity for osteoblasts as it was nonreactive in all nonbone cells. ON was not specific for osteoblasts but consistently immunostained other cell types in our EOSA tumors: fibroblasts (100%), pericytes (96%), endothelial cells (92%), chondrocytes (5/5), basal layer of skin epithelium (1/4), nerves (2/2), and osteoclastic giant cells (64%). ON also stained several other cell types in normal and neoplastic tissues in our battery of preliminary stainings; OC was negative in all nonosteoblastic tissues and tumors. Both OC and ON were specific for osteoid matrix as they were nonreactive in both collagen and cartilage matrix. OC is a sensitive and specific marker for bone cells and would be helpful in identifying EOSA, even in the absence of neoplastic bone on small biopsies. ON and OC (more sensitive) will both distinguish malignant bone from collagen and cartilage matrix, essential to the diagnosis of EOSA.

摘要

骨外骨肉瘤(EOSA)是一种罕见的恶性软组织肿瘤,根据定义,它不附着于骨骼,由产生骨基质(即肿瘤性骨)的成骨细胞表型的恶性细胞组成。由于其位置关系,它可能会与其他软组织肿瘤相似,其基质也可能被误认为是玻璃样变的胶原。我们研究了抗骨钙素(OC)和抗骨连接蛋白(ON)这两种针对两种丰富的人类骨蛋白的抗体在骨外骨肉瘤诊断中的应用。从武装部队病理研究所(华盛顿特区)的软组织登记处识别出28例编码为骨外骨肉瘤(n = 24)或可能为骨外骨肉瘤(n = 4)的病例。所有病例都有用于免疫组织化学的石蜡块。对肿瘤细胞和基质进行OC和ON(Biodesign International,缅因州肯纳邦克,克隆OC1和OST1)免疫染色,并根据四级分级系统进行分级:1 = 局灶性(<50%)弱染色;2 = 局灶性强染色;3 = 弥漫性(≥50%)弱染色;4 = 弥漫性强染色。患者年龄从9岁到80岁不等,平均年龄为57岁。有9例女性患者和19例男性患者。肿瘤大小从1.5厘米到15厘米不等,平均大小为5.8厘米。部位包括下肢(n = 14)、躯干(n = 9)、上肢(n = 4)和头颈部(n = 1)。亚型包括12例成骨细胞型、4例纤维母细胞型、2例软骨母细胞型、2例高分化型、1例毛细血管扩张型、1例小细胞型和6例富含巨细胞的骨外骨肉瘤;后者类似于伴有肿瘤性骨形成的富含巨细胞的恶性纤维组织细胞瘤。所有肿瘤都有肿瘤细胞和骨肿瘤基质可供评估。OC对骨外骨肉瘤肿瘤细胞的敏感性为82%(1至4+),91%的病例中远离骨的肿瘤细胞有免疫染色,对骨肿瘤基质的敏感性为75%(2至4+)。ON对骨外骨肉瘤肿瘤细胞的敏感性为93%(2至4+),而对骨肿瘤基质的敏感性仅为39%(1至4+)。在100%富含巨细胞的骨外骨肉瘤中,肿瘤细胞对OC和ON呈阳性(2至4+)。OC对成骨细胞具有100%的特异性,因为它在所有非骨细胞中均无反应。ON对成骨细胞不具有特异性,但在我们的骨外骨肉瘤肿瘤中始终对其他细胞类型进行免疫染色:纤维母细胞(100%)、周细胞(96%)、内皮细胞(92%)、软骨细胞(5/5)、皮肤上皮基底层(1/4)、神经(2/2)和破骨巨细胞(64%)。在我们一系列初步染色中,ON也对正常组织和肿瘤组织中的其他几种细胞类型进行染色;OC在所有非成骨细胞组织和肿瘤中均为阴性。OC和ON对类骨质基质均具有特异性,因为它们在胶原和软骨基质中均无反应。OC是骨细胞的一种敏感且特异的标志物,即使在小活检中没有肿瘤性骨的情况下,也有助于识别骨外骨肉瘤。ON和OC(更敏感)都能将恶性骨与胶原和软骨基质区分开来,这对骨外骨肉瘤的诊断至关重要。

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