Department of Anatomical and Cellular Pathology, The Chinese University of Hong Kong, Shatin, Hong Kong.
Department of Pathology, The First Affiliated Hospital of Zhengzhou University, Zhengzhou, China.
Acta Neuropathol Commun. 2020 Nov 10;8(1):191. doi: 10.1186/s40478-020-01066-6.
Adult medulloblastomas are clinically and molecularly understudied due to their rarity. We performed molecular grouping, targeted sequencing, and TERT promoter Sanger sequencing on a cohort of 99 adult medulloblastomas. SHH made up 50% of the cohort, whereas Group 3 (13%) was present in comparable proportion to WNT (19%) and Group 4 (18%). In contrast to paediatric medulloblastomas, molecular groups had no prognostic impact in our adult cohort (p = 0.877). Most frequently mutated genes were TERT (including promoter mutations, mutated in 36% cases), chromatin modifiers KMT2D (31%) and KMT2C (30%), TCF4 (31%), PTCH1 (27%) and DDX3X (24%). Adult WNT patients showed enrichment of TP53 mutations (6/15 WNT cases), and 3/6 TP53-mutant WNT tumours were of large cell/anaplastic histology. Adult SHH medulloblastomas had frequent upstream pathway alterations (PTCH1 and SMO mutations) and few downstream alterations (SUFU mutations, MYCN amplifications). TERT promoter mutations were found in 72% of adult SHH patients, and were restricted to this group. Adult Group 3 tumours lacked hallmark MYC amplifications, but had recurrent mutations in KBTBD4 and NOTCH1. Adult Group 4 tumours harboured recurrent mutations in TCF4 and chromatin modifier genes. Overall, amplifications of MYC and MYCN were rare (3%). Since molecular groups were not prognostic, alternative prognostic markers are needed for adult medulloblastoma. KMT2C mutations were frequently found across molecular groups and were associated with poor survival (p = 0.002). Multivariate analysis identified histological type (p = 0.026), metastasis (p = 0.031) and KMT2C mutational status (p = 0.046) as independent prognosticators in our cohort. In summary, we identified distinct clinical and mutational characteristics of adult medulloblastomas that will inform their risk stratification and treatment.
成人髓母细胞瘤由于其罕见性,在临床和分子水平上的研究都较少。我们对 99 例成人髓母细胞瘤进行了分子分组、靶向测序和 TERT 启动子 Sanger 测序。SHH 占队列的 50%,而 Group 3(13%)与 WNT(19%)和 Group 4(18%)的比例相当。与儿童髓母细胞瘤不同,分子分组在我们的成人队列中没有预后影响(p=0.877)。最常突变的基因是 TERT(包括启动子突变,在 36%的病例中突变)、染色质修饰因子 KMT2D(31%)和 KMT2C(30%)、TCF4(31%)、PTCH1(27%)和 DDX3X(24%)。成人 WNT 患者中 TP53 突变富集(15 例 WNT 患者中有 6 例),且 6 例 TP53 突变的 WNT 肿瘤中有 3 例为大细胞/间变性组织学。成人 SHH 髓母细胞瘤常有上游通路改变(PTCH1 和 SMO 突变),下游改变较少(SUFU 突变,MYCN 扩增)。72%的成人 SHH 患者存在 TERT 启动子突变,且仅限于该组。成人 Group 3 肿瘤缺乏标志性的 MYC 扩增,但有 KBTBD4 和 NOTCH1 的反复突变。成人 Group 4 肿瘤存在 TCF4 和染色质修饰基因的反复突变。总体而言,MYC 和 MYCN 的扩增很少见(3%)。由于分子分组不是预后因素,因此需要为成人髓母细胞瘤寻找替代的预后标志物。KMT2C 突变在各分子组中均频繁发生,且与生存率差相关(p=0.002)。多变量分析确定了组织学类型(p=0.026)、转移(p=0.031)和 KMT2C 突变状态(p=0.046)是我们队列中的独立预后因素。总之,我们确定了成人髓母细胞瘤的独特临床和突变特征,这将为其风险分层和治疗提供信息。
