Department of Pathology and Laboratory Medicine, McGovern Medical School, The University of Texas Health Science Center at Houston, Houston, TX, USA.
Vivian L. Smith Department of Neurosurgery, McGovern Medical School, The University of Texas Health Science Center at Houston, Houston, TX, USA.
J Neurooncol. 2020 Sep;149(3):463-472. doi: 10.1007/s11060-020-03634-1. Epub 2020 Oct 3.
Recently, the term "Diffuse glioma, BRAF V600E-mutant" has been recommended for IDH-wildtype gliomas with BRAF p.V600E mutation and without CDKN2A/B deletion. However, additional alterations in gliomas that coexist with BRAF-mutations are poorly defined.
We analyzed next-generation sequencing results in 315 cancer-associated genes for 372 gliomas from our institution (2010 to 2017). In addition, we reviewed IDH-WT gliomas with mutation and copy-number alterations available in cBioPortal, to further characterize BRAF-mutant gliomas.
Seventeen (4.6%) showed BRAF mutations. Tumor types included 8 glioblastomas, 2 epithelioid glioblastomas (E-GBM), 2 pleomorphic xanthoastrocytomas (PXA), 1 anaplastic oligodendroglioma, 1 diffuse astrocytoma, and 3 pilocytic astrocytomas. Fifty-three percent (53%) of cases exhibited BRAF-alterations other than p.V600E. The majority of the tumors were localized in the temporal lobe (52.9%). In addition to BRAF mutations, glioblastomas showed concomitant mutations in TP53 (3/8), CDKN2A/B-loss (6/8), TERT-promoter (6/8), and/or PTEN (5/8). Both E-GBMs and PXAs showed CDKN2A/B-loss and BRAF p.V600E with absence of TERTp, TP53, and PTEN mutations. Similar findings were observed in BRAF-mutant infiltrating gliomas from cBioPortal.
Knowledge of additional alterations that co-occur with BRAF-mutations in gliomas may improve diagnosis and help identify patients that could benefit from targeted therapies. Furthermore, we provide examples of two patients whose tumors responded to BRAF pathway inhibitors, arguing in favor of these therapies in patients with BRAF-mutant gliomas.
最近,术语“弥漫性脑胶质瘤,BRAF V600E 突变型”被推荐用于 IDH 野生型伴 BRAF p.V600E 突变且无 CDKN2A/B 缺失的胶质瘤。然而,与 BRAF 突变共存的胶质瘤中的其他改变尚不清楚。
我们分析了本机构的 315 种癌症相关基因的下一代测序结果,共涉及 372 例胶质瘤(2010 年至 2017 年)。此外,我们还在 cBioPortal 中回顾了 IDH-WT 胶质瘤中可获得的突变和拷贝数改变,以进一步表征 BRAF 突变型胶质瘤。
17 例(4.6%)显示 BRAF 突变。肿瘤类型包括 8 例胶质母细胞瘤、2 例上皮样胶质母细胞瘤(E-GBM)、2 例多形性黄色星形细胞瘤(PXA)、1 例间变性少突胶质细胞瘤、1 例弥漫性星形细胞瘤和 3 例毛细胞星形细胞瘤。53%(53%)的病例显示除 p.V600E 以外的 BRAF 改变。大多数肿瘤位于颞叶(52.9%)。除 BRAF 突变外,胶质母细胞瘤还显示 TP53(3/8)、CDKN2A/B 缺失(6/8)、TERT 启动子(6/8)和/或 PTEN(5/8)的伴随突变。E-GBM 和 PXA 均显示 CDKN2A/B 缺失和 BRAF p.V600E,而 TERTp、TP53 和 PTEN 突变缺失。在 cBioPortal 中的 BRAF 突变浸润性胶质瘤中也观察到类似的发现。
了解 BRAF 突变型胶质瘤中同时发生的其他改变可能有助于提高诊断,并有助于识别可能受益于靶向治疗的患者。此外,我们提供了两名患者的肿瘤对 BRAF 通路抑制剂有反应的例子,支持在 BRAF 突变型胶质瘤患者中使用这些治疗方法。
