Department of Pathology and Clinical Laboratories, National Cancer Center Hospital, Tokyo, Japan.
Department of Pathology, The University of Tokyo, Tokyo, Japan.
Mod Pathol. 2019 Mar;32(3):435-445. doi: 10.1038/s41379-018-0140-5. Epub 2018 Oct 5.
Dedifferentiated chondrosarcoma is a rare bone sarcoma, whose genetic background remains incompletely understood. Mutations in SUZ12 or EED, which encode polycomb repressive complex 2 (PRC2) components, and resulting deficiency in H3K27me3 are characteristic features of the majority of malignant peripheral nerve sheath tumors. Here, we investigated H3K27me3 and PRC2 status in dedifferentiated chondrosarcoma. Among 19 evaluable dedifferentiated chondrosarcoma cases, six (32%) showed immunohistochemical loss of H3K27me3 only in the dedifferentiated component, whereas the well-differentiated component retained H3K27me3. H3K27me3-deficient dedifferentiated chondrosarcoma occurred in two men and four women with a median age of 66. All of these tumors affected bones of the upper half of the body, with the ribs being preferentially involved, which represented a significantly different distribution compared to that in the 13 H3K27me3-intact dedifferentiated chondrosarcomas. H3K27me3-deficient dedifferentiated chondrosarcomas were histologically different from H3K27me3-intact dedifferentiated chondrosarcomas, as the former invariably demonstrated dedifferentiated histology with a striking similarity to classic malignant peripheral nerve sheath tumor, comprising sweeping to swirling fascicles of relatively uniform spindle cells. Heterologous rhabdomyoblastic differentiation, the focal presence of grade 3 chondrosarcoma histology, and a cartilaginous component in the metastatic sites were exclusively seen in some cases of H3K27me3-deficient dedifferentiated chondrosarcoma. In all three H3K27me3-deficient dedifferentiated chondrosarcomas that contained focal grade 3 histology, dedifferentiated components did not juxtapose to the grade 3 areas but transitioned abruptly from the grade 1-2 components. Targeted next generation sequencing, which was successfully performed on four H3K27me3-deficient dedifferentiated chondrosarcomas, identified an IDH2 mutation in one case and COL2A1 truncations in three cases. The dedifferentiated areas of three cases harbored SUZ12 or EED alterations, which were absent in the well-differentiated component, suggesting a role for PRC2 aberrations in dedifferentiation. H3K27me3 deficiency defines a novel subset of dedifferentiated chondrosarcoma that requires recognition because of its diagnostic and potential clinical implications.
去分化软骨肉瘤是一种罕见的骨肉瘤,其遗传背景仍不完全清楚。SUZ12 或 EED 的突变,其编码多梳抑制复合物 2(PRC2)成分,以及由此导致的 H3K27me3 的缺乏,是大多数恶性外周神经鞘肿瘤的特征。在这里,我们研究了去分化软骨肉瘤中的 H3K27me3 和 PRC2 状态。在 19 例可评估的去分化软骨肉瘤病例中,有 6 例(32%)仅在去分化成分中显示 H3K27me3 的免疫组织化学缺失,而分化良好的成分保留了 H3K27me3。在两名男性和四名女性中发现 H3K27me3 缺陷型去分化软骨肉瘤,中位年龄为 66 岁。所有这些肿瘤均影响上半身的骨骼,肋骨优先受累,这与 13 例 H3K27me3 完整的去分化软骨肉瘤的分布有显著差异。H3K27me3 缺陷型去分化软骨肉瘤在组织学上与 H3K27me3 完整的去分化软骨肉瘤不同,因为前者总是表现出与经典恶性外周神经鞘肿瘤明显相似的去分化组织学,包括相对均匀的梭形细胞的扫荡到漩涡状束。异源性横纹肌样分化、局灶性 3 级软骨肉瘤组织学和转移性部位的软骨成分仅见于一些 H3K27me3 缺陷型去分化软骨肉瘤病例中。在所有 3 例含有局灶性 3 级组织学的 H3K27me3 缺陷型去分化软骨肉瘤中,去分化成分与 3 级区域不相邻,而是从 1-2 级成分突然转变。对 4 例 H3K27me3 缺陷型去分化软骨肉瘤成功进行了靶向下一代测序,发现 1 例存在 IDH2 突变,3 例存在 COL2A1 截断。3 例的去分化区域存在 SUZ12 或 EED 改变,而在分化良好的成分中不存在,提示 PRC2 异常在去分化中起作用。H3K27me3 缺失定义了一种新的去分化软骨肉瘤亚组,由于其诊断和潜在的临床意义,需要加以认识。
