Molecular and clinical heterogeneity within MYC-family amplified medulloblastoma is associated with survival outcomes: A multicenter cohort study.

IF 16.4 1区 医学 Q1 CLINICAL NEUROLOGY Neuro-oncology Pub Date : 2024-10-08 DOI:10.1093/neuonc/noae178
Edward C Schwalbe, Janet C Lindsey, Marina Danilenko, Rebecca M Hill, Stephen Crosier, Sarra L Ryan, Daniel Williamson, Jemma Castle, Debbie Hicks, Marcel Kool, Till Milde, Andrey Korshunov, Stefan M Pfister, Simon Bailey, Steven C Clifford
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Abstract

Background: MYC/MYCN are the most frequent oncogene amplifications in medulloblastoma (MB) and its primary biomarkers of high-risk (HR) disease. However, while many patients' MYC(N)-amplified tumors are treatment-refractory, some achieve long-term survival. We therefore investigated clinicobiological heterogeneity within MYC(N)-amplified MB and determined its relevance for improved disease management.

Methods: We characterized the clinical and molecular correlates of MYC- (MYC-MB; n = 64) and MYCN-amplified MBs (MYCN-MB; n = 95), drawn from >1600 diagnostic cases.

Results: Most MYC-MBs were molecular group 3 (46/58; 79% assessable) and aged ≥3 years at diagnosis (44/64 [69%]). We identified a "canonical" very high-risk (VHR) MYC-amplified group (n = 51/62; 82%) with dismal survival irrespective of treatment (11% 5-year progression-free survival [PFS]), defined by co-occurrence with ≥1 additional established risk factor(s) (subtotal surgical-resection [STR], metastatic disease, LCA pathology), and commonly group 3/4 subgroup 2 with a high proportion of amplified cells. The majority of remaining noncanonical MYC-MBs survived (i.e. non-group 3/group 3 without other risk features; 11/62 (18%); 61% 5-year PFS). MYCN survival was primarily related to molecular group; MYCN-amplified SHH MB, and group 3/4 MB with additional risk factors, respectively defined VHR and HR groups (VHR, 39% [35/89]; 20% 5-year PFS/HR, 33% [29/89]; 46% 5-year PFS). Twenty-two out of 35 assessable MYCN-amplified SHH tumors harbored TP53 mutations; 9/12 (75%) with data were germline. MYCN-amplified group 3/4 MB with no other risk factors (28%; 25/89) had 70% 5-year PFS.

Conclusions: MYC(N)-amplified MB displays significant clinicobiological heterogeneity. Diagnostics incorporating molecular groups, subgroups, and clinical factors enable their risk assessment. VHR "canonical" MYC tumors are essentially incurable and SHH-MYCN-amplified MBs fare extremely poorly (20% survival at 5 years); both require urgent development of alternative treatment strategies. Conventional risk-adapted therapies are appropriate for more responsive groups, such as noncanonical MYC and non-SHH-MYCN MB.

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MYC家族扩增髓母细胞瘤的分子和临床异质性与生存结果相关:一项多中心队列研究。
背景:MYC/MYCN是髓母细胞瘤(MB)中最常见的癌基因扩增,也是高风险(HR)疾病的主要生物标志物。然而,虽然许多患者的MYC(N)扩增肿瘤具有治疗难治性,但也有一些患者获得了长期生存。因此,我们研究了MYC(N)扩增MB的临床生物学异质性,并确定其与改善疾病管理的相关性:方法:我们从超过 1600 例诊断病例中提取了 MYC-(MYC-MB;n = 64)和 MYCN-扩增 MB(MYCN-MB;n = 95)的临床和分子相关性特征:大多数 MYC-MB 属于分子第 3 组(46/58;79% 可评估),诊断时年龄≥3 岁(44/64 [69%])。我们发现了一个 "典型的 "极高风险(VHR)MYC扩增组(n = 51/62;82%),该组无论治疗与否,生存率都很低(5年无进展生存率[PFS]为11%),其定义是同时存在≥1个额外的既定风险因素(次全手术切除[STR]、转移性疾病、LCA病理),而且通常是扩增细胞比例较高的3/4亚组2。其余大多数非典型 MYC-MB 存活下来(即非第 3 组/无其他风险特征的第 3 组;11/62(18%);61% 的 5 年 PFS)。MYCN 存活率主要与分子组别有关;MYCN 扩增的 SHH MB 和具有其他风险因素的 3/4 组 MB 分别定义为 VHR 组和 HR 组(VHR,39% [35/89];20% 5 年 PFS/HR,33% [29/89];46% 5 年 PFS)。35例可评估的MYCN扩增SHH肿瘤中有22例携带TP53突变,其中9/12(75%)例携带种系突变数据。无其他风险因素的MYCN扩增3/4组MB(28%;25/89)的5年生存率为70%:结论:MYC(N)扩增MB显示出显著的临床生物学异质性。结合分子组、亚组和临床因素的诊断方法可对其进行风险评估。VHR "典型 "MYC肿瘤基本上是不可治愈的,而SHH-MYCN扩增的MBs的治疗效果极差(5年生存率为20%);两者都迫切需要开发替代治疗策略。传统的风险适应疗法适用于反应较快的群体,如非典型 MYC 和非 SHH-MYCN MB。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Neuro-oncology
Neuro-oncology 医学-临床神经学
CiteScore
27.20
自引率
6.30%
发文量
1434
审稿时长
3-8 weeks
期刊介绍: Neuro-Oncology, the official journal of the Society for Neuro-Oncology, has been published monthly since January 2010. Affiliated with the Japan Society for Neuro-Oncology and the European Association of Neuro-Oncology, it is a global leader in the field. The journal is committed to swiftly disseminating high-quality information across all areas of neuro-oncology. It features peer-reviewed articles, reviews, symposia on various topics, abstracts from annual meetings, and updates from neuro-oncology societies worldwide.
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