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Review
. 2022 Apr 30;14(9):2256.
doi: 10.3390/cancers14092256.

Clinical Significance of Molecular Alterations and Systemic Therapy for Meningiomas: Where Do We Stand?

Alessia Pellerino  1 Francesco Bruno  1 Rosa Palmiero  1 Edoardo Pronello  2 Luca Bertero  3 Riccardo Soffietti  1 Roberta Rudà  1   4
Affiliations
Review

Clinical Significance of Molecular Alterations and Systemic Therapy for Meningiomas: Where Do We Stand?

Alessia Pellerino et al. Cancers (Basel). .

Abstract

Meningiomas are common intracranial tumors that can be treated successfully in most cases with surgical resection and/or adjuvant radiotherapy. However, approximately 20% of patients show an aggressive clinical course with tumor recurrence or progressive disease, resulting in significant morbidity and increased mortality. Despite several studies that have investigated different cytotoxic agents in aggressive meningiomas in the past several years, limited evidence of efficacy and clinical benefit has been reported thus far. Novel molecular alterations have been linked to a particular clinicopathological phenotype and have been correlated with grading, location, and prognosis of meningiomas. In this regard, SMO, AKT, and PIK3CA mutations are typical of anterior skull base meningiomas, whereas KLF4 mutations are specific for secretory histology, and BAP1 alterations are common in progressive rhabdoid meningiomas. Alterations in TERT, DMD, and BAP1 correlate with poor outcomes. Moreover, some actionable mutations, including SMO, AKT1, and PIK3CA, regulate meningioma growth and are under investigation in clinical trials. PD-L1 and/or M2 macrophage expression in the microenvironment provides evidence for the investigation of immunotherapy in progressive meningiomas.

Keywords: AKT; PIK3CA; SMO; chemotherapy; immunotherapy; recurrent meningioma.

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Conflict of interest statement

A.P. declares no conflicts of interest; F.B. declares no conflicts of interest; R.P. declares no conflicts of interest; E.P. declares no conflicts of interest; L.B. declares no conflicts of interest; R.S declares the following financial disclosure: AstraZeneca, Merck and Orbus e Agios Therapeutics.; R.R. declares the following financial disclosure: UCB, Mundipharma, Bayer, and Novocure.

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