Canonical Amplifications and CDKN2A/B Loss Refine IDH1/2-mutant Astrocytoma Prognosis.

IF 16.4 1区医学 Q1 CLINICAL NEUROLOGY

Neuro-oncology Pub Date : 2024-11-25 DOI:10.1093/neuonc/noae258

Hia S Ghosh, Ruchit V Patel, Elizabeth B Claus, L Nicolas Gonzalez Castro, Patrick Y Wen, Keith L Ligon, David M Meredith, Wenya Linda Bi

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引用次数: 0

Abstract

Background: Molecular features have been incorporated alongside histologic criteria to improve glioma diagnostics and prognostication. CDKN2A/B homozygous-loss associates with worse survival in IDH1/2-mutant astrocytomas (IDHmut-astrocytomas), the presence of which denotes grade 4 tumor independent of histologic features. However, no molecular features distinguish survival amongst histologically-defined grade 2 and 3 IDHmut-astrocytomas.

Methods: We assembled a cohort of patients ≥19 years old diagnosed with an IDHmut-astrocytoma between 1989-2020 from public datasets and several academic medical centers. Multivariate modeling and unbiased clustering were used to stratify risk.

Results: We identified 998 IDHmut-astrocytoma patients (41.5% female; 85.6% white). Tumor grade, CDKN2A/B loss, and/or ≥1 focal amplification was associated with reduced survival. Grade 2/3 patients with intact CDKN2A/B and no focal amplifications survived the longest (OS 205.7 months). Survival for grade 2/3 cases with either CDKN2A/B hemizygous-loss or focal amplifications (80.4, 88.7 months respectively) did not differ significantly from grade 4 cases with intact CDKN2A/B and no amplifications (91.5 months, p=0.93). Grade 4 patients with either hemizygous or homozygous loss of CDKN2A/B had the shortest survival (OS 31.9, 32.5 months respectively), followed by grade 4 cases with intact CDKN2A/B and focal gene amplifications (OS 55.9 months). Integrating CDKN2A/B status and amplifications alongside histopathologic grade refined overall survival prediction. Unbiased clustering revealed 9 distinct molecular profiles, with differential survival. IDHmut-astrocytomas with any CDKN2A/B-loss clustered together, regardless of grade, and exhibited the poorest outcomes.

Conclusions: Combining CDKN2A/B hemizygous-loss and focal gene amplifications reveals a group of IDHmut-astrocytoma patients with intermediate prognosis, refining IDHmut-astrocytoma classification.

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典型扩增和 CDKN2A/B 缺失细化了 IDH1/2 突变星形细胞瘤的预后。

背景：分子特征已被纳入组织学标准，以改善胶质瘤的诊断和预后。CDKN2A/B同基因缺失与IDH1/2突变星形细胞瘤（IDHmut-astrocytomas）的生存率降低有关，CDKN2A/B同基因缺失表示肿瘤为4级，与组织学特征无关。然而，在组织学定义的2级和3级IDHmut-星形细胞瘤中，没有任何分子特征能区分生存率：我们从公共数据集和几个学术医疗中心收集了1989-2020年间被诊断为IDHmut-胃细胞瘤的≥19岁的患者队列。采用多变量建模和无偏聚类对风险进行分层：我们发现了998名IDHmut-胃细胞瘤患者（41.5%为女性；85.6%为白人）。肿瘤分级、CDKN2A/B缺失和/或≥1个病灶扩增与生存率降低有关。CDKN2A/B完整且无局灶性扩增的2/3级患者存活时间最长（OS 205.7个月）。CDKN2A/B半卵球形缺失或局灶性扩增的2/3级病例的生存期（分别为80.4个月和88.7个月）与CDKN2A/B完整且无扩增的4级病例（91.5个月，P=0.93）无显著差异。CDKN2A/B半杂合子或同卵合子缺失的4级患者生存期最短（OS分别为31.9个月和32.5个月），其次是CDKN2A/B完整且存在局灶性基因扩增的4级病例（OS为55.9个月）。将CDKN2A/B状态和基因扩增与组织病理学分级结合起来，可完善总生存期预测。无偏聚类显示了9种不同的分子特征，其生存期也有所不同。具有任何CDKN2A/B缺失的IDHmut-胃细胞瘤聚集在一起，无论其分级如何，均表现出最差的预后：结论：结合CDKN2A/B半基因缺失和局灶基因扩增，可发现一组预后居中的IDHmut-胃细胞瘤患者，从而完善了IDHmut-胃细胞瘤的分类。

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 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.