Methylation-based classification of benign and malignant peripheral nerve sheath tumors

被引:130
|
作者
Roehrich, Manuel [1 ,2 ]
Koelsche, Christian [1 ,2 ]
Schrimpf, Daniel [1 ,2 ]
Capper, David [1 ,2 ]
Sahm, Felix [1 ,2 ]
Kratz, Annekathrin [1 ,2 ]
Reuss, Jana [2 ]
Hovestadt, Volker [3 ]
Jones, David T. W. [4 ]
Bewerunge-Hudler, Melanie [5 ]
Becker, Albert [6 ]
Weis, Joachim [7 ]
Mawrin, Christian [8 ]
Mittelbronn, Michel [9 ,10 ,11 ]
Perry, Arie [12 ]
Mautner, Victor-Felix [13 ]
Mechtersheimer, Gunhild [14 ]
Hartmann, Christian [15 ]
Okuducu, Ali Fuat [16 ]
Arp, Mirko [17 ]
Seiz-Rosenhagen, Marcel [17 ]
Haenggi, Daniel [17 ]
Heim, Stefanie [18 ]
Paulus, Werner [18 ]
Schittenhelm, Jens [19 ]
Ahmadi, Rezvan [20 ]
Herold-Mende, Christel [20 ]
Unterberg, Andreas [20 ]
Pfister, Stefan M. [4 ,21 ]
von Deimling, Andreas [1 ,2 ]
Reuss, David E. [1 ,2 ]
机构
[1] Heidelberg Univ, Inst Pathol, Dept Neuropathol, Neuenheimer Feld 220, Heidelberg, Germany
[2] German Canc Res Ctr, German Canc Consortium DKTK, Clin Cooperat Unit Neuropathol, Heidelberg, Germany
[3] German Canc Res Ctr, German Canc Consortium DKTK, Div Mol Genet, Heidelberg, Germany
[4] German Canc Res Ctr, Div Pediat Neurooncol, German Canc Consortium DKTK, Heidelberg, Germany
[5] German Canc Res Ctr, Genom & Prote Core Facil, INF 580, Microarray Unit, Heidelberg, Germany
[6] Univ Med Ctr, Inst Neuropathol, Bonn, Germany
[7] Aachen Univ Hosp, Rhein Westfal Tech Hsch, Inst Neuropathol, Aachen, Germany
[8] Univ Magdeburg, Dept Neuropathol, D-39106 Magdeburg, Germany
[9] Goethe Univ Frankfurt, Inst Neurol, Edinger Inst, D-60054 Frankfurt, Germany
[10] German Canc Consortium DKTK, Heidelberg, Germany
[11] German Canc Res Ctr, Heidelberg, Germany
[12] Univ Calif San Francisco, Div Neuropathol, San Francisco, CA 94143 USA
[13] Univ Hosp Hamburg Eppendorf, Dept Neurol, D-20246 Hamburg, Germany
[14] Heidelberg Univ, Inst Pathol, Dept Gen Pathol, Heidelberg, Germany
[15] Hannover Med Sch, Dept Neuropathol, Hannover, Germany
[16] Municipal Hosp Nurnberg, Dept Pathol, Nurnberg, Germany
[17] Heidelberg Univ, Med Fac Mannheim, Univ Med Mannheim, Dept Neurosurg, Mannheim, Germany
[18] Univ Hosp, Inst Neuropathol, Munster, Germany
[19] Univ Hosp, Dept Neuropathol, Tubingen, Germany
[20] Heidelberg Univ, Dept Neurosurg, Heidelberg, Germany
[21] Univ Med Ctr, Dept Pediat Oncol Hematol & Immunol, Heidelberg, Germany
来源
ACTA NEUROPATHOLOGICA | 2016年 / 131卷 / 06期
关键词
MPNST; Atypical neurofibroma; Schwannoma; Ganglioneuroma; Peripheral nerve sheath tumor; Methylation; 450k; PRC2; NF1; Clone NFC; H3K27me3; DNA METHYLATION; CELL; MUTATIONS; FUSION; ORIGIN; MYXOMA; MPNST; SUZ12; PRC2;
D O I
10.1007/s00401-016-1540-6
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
The vast majority of peripheral nerve sheath tumors derive from the Schwann cell lineage and comprise diverse histological entities ranging from benign schwannomas and neurofibromas to high-grade malignant peripheral nerve sheath tumors (MPNST), each with several variants. There is increasing evidence for methylation profiling being able to delineate biologically relevant tumor groups even within the same cellular lineage. Therefore, we used DNA methylation arrays for methylome- and chromosomal profile-based characterization of 171 peripheral nerve sheath tumors. We analyzed 28 conventional high-grade MPNST, three malignant Triton tumors, six low-grade MPNST, four epithelioid MPNST, 33 neurofibromas (15 dermal, 8 intraneural, 10 plexiform), six atypical neurofibromas, 43 schwannomas (including 5 NF2 and 5 schwannomatosis associated cases), 11 cellular schwannomas, 10 melanotic schwannomas, 7 neurofibroma/schwannoma hybrid tumors, 10 nerve sheath myxomas and 10 ganglioneuromas. Schwannomas formed different epigenomic subgroups including a vestibular schwannoma subgroup. Cellular schwannomas were not distinct from conventional schwannomas. Nerve sheath myxomas and neurofibroma/schwannoma hybrid tumors were most similar to schwannomas. Dermal, intraneural and plexiform neurofibromas as well as ganglioneuromas all showed distinct methylation profiles. Atypical neurofibromas and low-grade MPNST were indistinguishable with a common methylation profile and frequent losses of CDKN2A. Epigenomic analysis finds two groups of conventional high-grade MPNST sharing a frequent loss of neurofibromin. The larger of the two groups shows an additional loss of trimethylation of histone H3 at lysine 27 (H3K27me3). The smaller one retains H3K27me3 and is found in spinal locations. Sporadic MPNST with retained neurofibromin expression did not form an epigenetic group and most cases could be reclassified as cellular schwannomas or soft tissue sarcomas. Widespread immunohistochemical loss of H3K27me3 was exclusively seen in MPNST of the main methylation cluster, which defines it as an additional useful marker for the differentiation of cellular schwannoma and MPNST.
引用
收藏
页码:877 / 887
页数:11
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