Loss of H3K27me3 in WHO grade 3 meningioma

被引:0
|
作者
Andrea Daniela Maier
Christian Beltoft Brøchner
Christian Mirian
Jeppe Haslund-Vinding
Jiri Bartek
Tomas J. Ekström
Frantz Rom Poulsen
David Scheie
Tiit Mathiesen
机构
[1] Copenhagen University Hospital,Department of Neurosurgery
[2] Rigshospitalet,Pathology Department
[3] Copenhagen University Hospital,Department of Neurosurgery
[4] Rigshospitalet,Department of Clinical Neuroscience
[5] Karolinska University Hospital,Center for Molecular Medicine
[6] Karolinska Institutet,Department of Molecular Medicine and Surgery
[7] Karolinska University Hospital,Department of Neurosurgery
[8] Karolinska Institutet,Clinical Institute
[9] Odense University Hospital,Department of Clinical Medicine
[10] University of Southern Denmark and BRIDGE,undefined
[11] University of Copenhagen,undefined
来源
Brain Tumor Pathology | 2022年 / 39卷
关键词
Meningioma; H3K27me3; Heterogeneity;
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中图分类号
学科分类号
摘要
Immunohistochemical quantification of H3K27me3 was reported to distinguish meningioma patients with an unfavorable prognosis but is not yet established as a prognostic biomarker within WHO grade 3 meningiomas. We studied H3K27me3 loss in a series of biopsies from primary and secondary malignant meningioma to validate its prognostic performance and describe if loss of H3K27me3 occurs during malignant transformation. Two observers quantified H3K27me3 status as “complete loss”, < 50% and > 50% stained cells in 110 tumor samples from a population-based consecutive cohort of 40 WHO grade 3 meningioma patients. We found no difference in overall survival (OS) in patients with > 50% H3K27me3 retention compared to < 50% in the cohort of patients with WHO grade 3 meningioma (Wald test p = 0.5). H3K27me3 staining showed heterogeneity in full section tumor slides while staining of the Barr body and peri-necrotic cells complicated quantification further. H3K27me3 expression differed without a discernible pattern between biopsies from repeated surgeries of meningioma recurrences. In conclusion, our results were not compatible with a systematic pattern of immunohistochemical H3K27me3 loss being associated with OS or malignant transformation of meningiomas and did not support H3K27me3 loss as a useful immunohistochemical biomarker within grade 3 meningiomas due to staining-specific challenges in quantification.
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页码:200 / 209
页数:9
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