The multiomic landscape of meningiomas: a review and update

Wang, Justin Z; Nassiri, Farshad; Landry, Alexander; Patil, Vikas; Liu, Jeff; Aldape, Kenneth; Gao, Andrew; Zadeh, Gelareh

doi:10.1007/s11060-023-04253-2

Cited by 6 publications

(8 citation statements)

References 65 publications

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“…Deletions of CDKN2A/B were detected three times (2 homozygous losses and 1 heterozygous loss), 1p loss 23 times (60.5%) and 22q losses 29 times (76.3%). The frequency of observed events was generally similar to larger meningioma cohorts [ 10 ]. Most cases were identified as intermediate meningioma MC (44.7%), followed by malignant (28.9%) and benign (26.3%) MC (molecular events per MC in Suppl.…”

supporting

confidence: 60%

“…Specifically, mutations in the promotor area of the telomerase reverse transcriptase ( TERT ) gene and/or homozygous loss of the CDKN2A/B locus automatically result in a grade 3 diagnosis [ 3 , 4 ]. Simultaneously meningioma with TRAF7 , AKT1 , KLF4 , and/or SMO mutations are, in general, associated with lower progression risk [ 1 , 10 ]. Alterations linked with increased risk include BAP1 mutations [ 9 ], copy-number variations of chromosomal arms such as 1p, 6q, 10q and 14q [ 6 ], genome-wide epigenetic profiles also referred to as DNA methylation classes (MC) [ 8 ], or the combination of molecular alterations included in an integrated risk score, grade or classification [ 2 , 5 , 7 ].…”

mentioning

confidence: 99%

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Independent prognostic impact of DNA methylation class and chromosome 1p loss in WHO grade 2 and 3 meningioma undergoing adjuvant high-dose radiotherapy: comprehensive molecular analysis of EORTC 22042–26042

Maas,

Sievers,

Weber

et al. 2023

Acta Neuropathol

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supporting

confidence: 60%

mentioning

confidence: 99%

Independent prognostic impact of DNA methylation class and chromosome 1p loss in WHO grade 2 and 3 meningioma undergoing adjuvant high-dose radiotherapy: comprehensive molecular analysis of EORTC 22042–26042

Maas,

Sievers,

Weber

et al. 2023

Acta Neuropathol

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“…Beyond the malignancy and other issues, recent years have seen much overall progress in meningioma genetics and molecular biology in general [ 63 ]. It appears that not all meningiomas are the same, and future meningioma classifications may be need to based at least in part on molecular and genetic parameters [ 29 , 48 , 65 ].…”

Section: Problems With Grading the Extent Of Meningioma Resectionsmentioning

confidence: 99%

Grading meningioma resections: the Simpson classification and beyond

Simon,

Gousias

2024

Acta Neurochir

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Technological (and also methodological) advances in neurosurgery and neuroimaging have prompted a reappraisal of Simpson’s grading of the extent of meningioma resections. To the authors, the published evidence supports the tenets of this classification. Meningioma is an often surgically curable dura-based disease. An extent of meningioma resection classification needs to account for a clinically meaningful variation of the risk of recurrence depending on the aggressiveness of the management of the (dural) tumor origin.Nevertheless, the 1957 Simpson classification undoubtedly suffers from many limitations. Important issues include substantial problems with the applicability of the grading paradigm in different locations. Most notably, tumor location and growth pattern often determine the eventual extent of resection, i.e., the Simpson grading does not reflect what is surgically achievable. Another very significant problem is the inherent subjectivity of relying on individual intraoperative assessments. Neuroimaging advances such as the use of somatostatin receptor PET scanning may help to overcome this central problem. Tumor malignancy and biology in general certainly influence the role of the extent of resection but may not need to be incorporated in an actual extent of resection grading scheme as long as one does not aim at developing a prognostic score. Finally, all attempts at grading meningioma resections use tumor recurrence as the endpoint. However, especially in view of radiosurgery/radiotherapy options, the clinical significance of recurrent tumor growth varies greatly between cases.In summary, while the extent of resection certainly matters in meningioma surgery, grading resections remains controversial. Given the everyday clinical relevance of this issue, a multicenter prospective register or study effort is probably warranted (including a prominent focus on advanced neuroimaging).

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“…Multiple large-cohort sequencing studies have established the landscape of somatic mutations in meningiomas, identifying mutually exclusive genomic subgroups that account for over 80% of all cases [9,66,96,97]. Bi-allelic loss of the tumor suppressor NF2 is associated with approximately one-half of sporadic meningiomas and most syndromic cases.…”

Section: Somatic Mutationsmentioning

confidence: 99%

The Evolving Classification of Meningiomas: Integration of Molecular Discoveries to Inform Patient Care

Trybula,

Youngblood,

Karras

et al. 2024

Cancers

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Meningioma classification and treatment have evolved over the past eight decades. Since Bailey, Cushing, and Eisenhart’s description of meningiomas in the 1920s and 1930s, there have been continual advances in clinical stratification by histopathology, radiography and, most recently, molecular profiling, to improve prognostication and predict response to therapy. Precise and accurate classification is essential to optimizing management for patients with meningioma, which involves surveillance imaging, surgery, primary or adjuvant radiotherapy, and consideration for clinical trials. Currently, the World Health Organization (WHO) grade, extent of resection (EOR), and patient characteristics are used to guide management. While these have demonstrated reliability, a substantial number of seemingly benign lesions recur, suggesting opportunities for improvement of risk stratification. Furthermore, the role of adjuvant radiotherapy for grade 1 and 2 meningioma remains controversial. Over the last decade, numerous studies investigating the molecular drivers of clinical aggressiveness have been reported, with the identification of molecular markers that carry clinical implications as well as biomarkers of radiotherapy response. Here, we review the historical context of current practices, highlight recent molecular discoveries, and discuss the challenges of translating these findings into clinical practice.

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The multiomic landscape of meningiomas: a review and update

Cited by 6 publications

References 65 publications

Independent prognostic impact of DNA methylation class and chromosome 1p loss in WHO grade 2 and 3 meningioma undergoing adjuvant high-dose radiotherapy: comprehensive molecular analysis of EORTC 22042–26042

Independent prognostic impact of DNA methylation class and chromosome 1p loss in WHO grade 2 and 3 meningioma undergoing adjuvant high-dose radiotherapy: comprehensive molecular analysis of EORTC 22042–26042

Grading meningioma resections: the Simpson classification and beyond

The Evolving Classification of Meningiomas: Integration of Molecular Discoveries to Inform Patient Care

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