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世界卫生组织 2 级和 3 级脑膜瘤分子生物学和转化研究进展:文献综述。

Advances in Molecular Biological and Translational Studies in World Health Organization Grades 2 and 3 Meningiomas: A Literature Review.

机构信息

Department of Neurosurgery, Faculty of Medicine, The University of Tokyo.

Department of Neurosurgery, Kyorin University.

出版信息

Neurol Med Chir (Tokyo). 2022 Aug 15;62(8):347-360. doi: 10.2176/jns-nmc.2022-0114. Epub 2022 Jul 22.

Abstract

The treatment of World Health Organization (WHO) grades 2 and 3 meningiomas remains difficult and controversial. The pathogenesis of high-grade meningiomas was expected to be elucidated to improve treatment strategies. The molecular biology of meningiomas has been clarified in recent years. High-grade meningiomas have been linked to NF2 mutations and 22q deletion. CDKN2A/B homozygous deletion and TERT promoter mutations are independent prognostic factors for WHO grade 3 meningiomas. In addition to 22q loss, 1p, 14p, and 9q loss have been linked to high-grade meningiomas. Meningiomas enriched in copy number alterations may be biologically invasive. Furthermore, several new comprehensive classifications of meningiomas have been proposed based on these molecular biological features, including DNA methylation status. The new classifications may have implications for treatment strategies for refractory aggressive meningiomas because they provide a more accurate prognosis compared to the conventional WHO classification. Although several systemic therapies, including molecular targeted therapies, may be effective in treating refractory aggressive meningiomas, these drugs are being tested. Systemic drug therapy for meningioma is expected to be developed in the future. Thus, this review aims to discuss the distinct genomic alterations observed in WHO grade 2 and 3 meningiomas, as well as their diagnostic and therapeutic implications and systemic drug therapies for high-grade meningiomas.

摘要

世界卫生组织(WHO)分级 2 级和 3 级脑膜瘤的治疗仍然具有挑战性和争议性。为了改进治疗策略,人们期望阐明高级别脑膜瘤的发病机制。近年来,脑膜瘤的分子生物学已经得到阐明。高级别脑膜瘤与 NF2 突变和 22q 缺失有关。CDKN2A/B 纯合性缺失和 TERT 启动子突变是 WHO 3 级脑膜瘤的独立预后因素。除 22q 缺失外,1p、14p 和 9q 缺失也与高级别脑膜瘤有关。拷贝数改变丰富的脑膜瘤可能具有生物学侵袭性。此外,基于这些分子生物学特征,包括 DNA 甲基化状态,已经提出了几种新的脑膜瘤综合分类。与传统的 WHO 分类相比,新的分类可能对难治性侵袭性脑膜瘤的治疗策略具有重要意义,因为它们提供了更准确的预后。尽管几种全身治疗方法,包括分子靶向治疗,可能对治疗难治性侵袭性脑膜瘤有效,但这些药物正在进行测试。脑膜瘤的全身药物治疗预计将在未来得到发展。因此,本综述旨在讨论 WHO 分级 2 级和 3 级脑膜瘤中观察到的独特基因组改变,以及它们的诊断和治疗意义以及高级别脑膜瘤的全身药物治疗。

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