FGFR2融合神经胶质细胞和神经胶质细胞肿瘤的表型和表观遗传异质性。

IF 4 2区 医学 Q1 CLINICAL NEUROLOGY
Alice Métais, Volodia Dangouloff-Ros, Jeremy Garcia, Quentin Vannod-Michel, Marie Csanyi, Arnault Tauziède-Espariat, Romain Appay, Claude-Alain Maurage, Emmanuelle Uro-Coste, David Meyronet, Valérie Rigau, Audrey Rousseau, Guillaume Chotard, Jocelyne Hamelin, Gaelle Pierron, Carole Colin, Morgan Ollivier, Margaux Roques, Corentin Provost, Jean-Philippe Cottier, Johan Pallud, Fabrice Chrétien, Lelio Guida, Thomas Blauwblomme, Nathalie Boddaert, Pascale Varlet, Myriam Edjlali, Dominique Figarella-Branger
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引用次数: 0

摘要

目的:FGFR融合的中枢神经系统(CNS)肿瘤非常罕见,通常属于神经胶质细胞瘤和神经元肿瘤或儿科型弥漫性低级别胶质瘤谱系。在这一谱系中,FGFR2融合已被记录在通过DNA甲基化分析归类为多形性低级别幼年神经上皮肿瘤(PLNTY)的肿瘤中,这是最近描述的一种肿瘤类型。然而,在神经胶质细胞瘤中也有FGFR2融合的报道,这凸显了诊断标准的重叠和挑战:方法:我们调查了法国全国系列肿瘤中的FGFR2融合情况,这些肿瘤被送往RENOCLIP-LOC网络。我们全面分析了16例FGFR2融合胶质细胞瘤的组织学、放射学和分子数据,包括DNA甲基化图谱:大多数肿瘤位于颞叶或顶叶,中位诊断年龄为7岁[1-44]。癫痫是最常见的症状。5名患者肿瘤进展或复发,中位无进展生存期为22.6个月。记录的组织学表型有PLNTY、GG、MVNT或未分类肿瘤。表观遗传学分析无法正确区分FGFR2融合胶质细胞瘤中与GG和PLNTY甲基化类别相关的表观遗传学群集。然而,神经放射学检查发现了截然不同的神经放射学模式:结论:虽然通过组织病理学或DNA甲基化分析来划分FGFR2融合的神经胶质细胞肿瘤谱系中的肿瘤类型仍具有挑战性,但神经影像学数据揭示了两种可能与PLNTY和神经节胶质瘤相关的不同模式。然而,要证实这一假设,还需要更多包括大量组织放射分子数据的系列研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Phenotypic and epigenetic heterogeneity in FGFR2-fused glial and glioneuronal tumours.

Aims: FGFR-fused central nervous system (CNS) tumours are rare and are usually within the glioneuronal and neuronal tumours or the paediatric-type diffuse low-grade glioma spectrum. Among this spectrum, FGFR2 fusion has been documented in tumours classified by DNA-methylation profiling as polymorphous low-grade neuroepithelial tumours of the young (PLNTY), a recently described tumour type. However, FGFR2 fusions have also been reported in glioneuronal tumours, highlighting the overlapping diagnostic criteria and challenges.

Methods: We investigated the FGFR2 fusion landscape in a French national series of tumours sent to the RENOCLIP-LOC network. We comprehensively analysed histology, radiology and molecular data including DNA-methylation profiling for 16 FGFR2-fused glioneuronal tumours.

Results: Most tumours were located in the temporal or parietal lobe with a median age at diagnosis of 7 years [1-44]. Epilepsy was the most frequent symptom. Five patients had tumour progression or recurrence with a median progression-free survival of 22.6 months. Histological phenotypes corresponding to PLNTY, GG, MVNT or unclassified tumours were recorded. Epigenetic profiling could not properly distinguish epigenetic clusters related to the GG and PLNTY methylation classes among FGFR2-fused glioneuronal tumours. However, a neuroradiological review identified strikingly distinct neuroradiological patterns.

Conclusion: While delineating tumour types among the FGFR2-fused glioneuronal tumour spectrum, by histopathology or DNA-methylation profiling, remains challenging, neuroimaging data revealed two distinct patterns that could correlate to PLNTY and ganglioglioma. However, more series including extensive histo-radio-molecular data are needed to confirm this hypothesis.

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来源期刊
CiteScore
8.20
自引率
2.00%
发文量
87
审稿时长
6-12 weeks
期刊介绍: Neuropathology and Applied Neurobiology is an international journal for the publication of original papers, both clinical and experimental, on problems and pathological processes in neuropathology and muscle disease. Established in 1974, this reputable and well respected journal is an international journal sponsored by the British Neuropathological Society, one of the world leading societies for Neuropathology, pioneering research and scientific endeavour with a global membership base. Additionally members of the British Neuropathological Society get 50% off the cost of print colour on acceptance of their article.
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