Institute of Neuropathology, University Medical Center Hamburg-Eppendorf, Hamburg, Germany.
II. Medizinische Klinik und Poliklinik, University Medical Center Hamburg-Eppendorf, Hamburg, Germany.
Acta Neuropathol. 2020 Feb;139(2):305-318. doi: 10.1007/s00401-019-02090-0. Epub 2019 Nov 2.
According to the WHO classification, ependymal tumors are classified as subependymomas, myxopapillary ependymomas, classic ependymomas, anaplastic ependymomas, and RELA-fusion-positive ependymomas (RELA-EPN). Among classic ependymomas, the WHO defines rare histological variants, i.e., the clear cell, papillary, and tanycytic ependymoma. In parallel, global DNA methylation patterns distinguish nine molecular groups, some of which tightly overlap with histopathological subgroups. However, the match of the aforementioned histological variants to DNA methylation classes remains unclear. We analyzed histomorphology, clinical parameters, and global DNA methylation of tumors with the initial histological diagnoses of tanycytic (n = 12), clear cell (n = 14), or papillary ependymoma (n = 19). Forty percent of these tumors did not match to the epigenetic profile of ependymomas, using a previously published DNA methylation-based classifier for brain tumors. Instead, they were classified as low-grade glioma (n = 3), plexus tumor (n = 2), CNS high-grade neuroepithelial tumor with MN1 alteration (n = 2), papillary tumor of the pineal region (n = 2), neurocytoma (n = 1), or did not match to any known brain tumor methylation class (n = 8). Overall, integrated diagnosis had to be changed in 35.6% of cases as compared to the initial diagnosis. Among the tumors molecularly classified as ependymoma (27/45 cases), tanycytic ependymomas were mostly located in the spine (5/7 cases) and matched to spinal or myxopapillary ependymoma. 6/8 clear cell ependymomas were found supratentorially and fell into the methylation class of RELA-EPN. Papillary ependymomas with a positive ependymoma match (12/19 cases) showed either a "papillary" (n = 5), a "trabecular" (n = 1), or a "pseudo-papillary" (n = 6) growth pattern. The papillary growth pattern was strongly associated with the methylation class B of posterior fossa ependymoma (PFB, 5/5 cases) and tumors displayed DNA methylation sites that were significantly different when compared to PFB ependymomas without papillary growth. Tumors with pseudo-papillary histology matched to the methylation class of myxopapillary ependymoma (4/6 cases), whereas the trabecular case was anatomically and molecularly a spinal ependymoma. Our results show that the diagnosis of histological ependymoma variants is challenging and epigenetic profiles may improve diagnostic accuracy of these cases. Whereas clear cell and papillary ependymomas display correlations between localization, histology, and methylation, tanycytic ependymoma does not represent a molecularly distinct subgroup.
根据世界卫生组织(WHO)的分类,室管膜瘤分为室管膜下瘤、黏液乳头状室管膜瘤、经典型室管膜瘤、间变型室管膜瘤和 RELA 融合阳性室管膜瘤(RELA-EPN)。在经典型室管膜瘤中,WHO 定义了罕见的组织学变体,即透明细胞型、乳头型和促纤维增生型室管膜瘤。同时,全球 DNA 甲基化模式区分了九个分子群,其中一些与组织病理学亚群紧密重叠。然而,上述组织学变体与 DNA 甲基化类别的匹配情况仍不清楚。我们分析了初始组织学诊断为促纤维增生型(n=12)、透明细胞型(n=14)或乳头型室管膜瘤(n=19)的肿瘤的组织形态学、临床参数和全球 DNA 甲基化。40%的这些肿瘤与之前发表的基于 DNA 甲基化的脑肿瘤分类器不匹配。相反,它们被归类为低级别胶质瘤(n=3)、丛状肿瘤(n=2)、CNS 高级别神经上皮肿瘤伴 MN1 改变(n=2)、松果体区乳头瘤(n=2)、神经细胞瘤(n=1)或与任何已知的脑肿瘤甲基化类群不匹配(n=8)。总体而言,与初始诊断相比,35.6%的病例需要进行综合诊断改变。在分子上被归类为室管膜瘤的肿瘤(27/45 例)中,促纤维增生型室管膜瘤大多位于脊柱(7/7 例),与脊髓或黏液乳头状室管膜瘤相匹配。8/6 例透明细胞室管膜瘤位于幕上,属于 RELA-EPN 的甲基化类群。与室管膜瘤相匹配的 12/19 例乳头型室管膜瘤表现出“乳头型”(n=5)、“小梁型”(n=1)或“假乳头型”(n=6)生长模式。乳头型生长模式与后颅窝室管膜瘤(PFB)的甲基化类群 B 密切相关(5/5 例),且肿瘤显示的 DNA 甲基化位点与无乳头型生长的 PFB 室管膜瘤有显著差异。具有假乳头组织学的肿瘤与黏液乳头状室管膜瘤的甲基化类群相匹配(4/6 例),而小梁型病例在解剖学和分子学上是脊髓室管膜瘤。我们的结果表明,组织学室管膜瘤变体的诊断具有挑战性,表观遗传学特征可能会提高这些病例的诊断准确性。虽然透明细胞型和乳头型室管膜瘤显示出定位、组织学和甲基化之间的相关性,但促纤维增生型室管膜瘤并不代表一个分子上独特的亚群。
