甲基组分析对儿童和青少年中枢神经系统肿瘤诊断和治疗的影响:希腊人口研究

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摘要

背景世界卫生组织(WHO)最近公布的中枢神经系统(CNS)肿瘤分类认为,DNA甲基化分析是一种理想的诊断工具,对于某些诊断而言,是辅助传统组织病理学的必要诊断工具。方法在这项合作研究中,我们报告了希腊一系列中枢神经系统肿瘤儿童和青少年的 DNA 甲基化结果(2018-2023 年)。共使用海德堡脑肿瘤分类器的最新适用版本分析了 130 个肿瘤样本。结果经初步分析,80%(104/130)的样本达到校准分数(Cs)≥ 0.9,并与已建立的甲基化类族/亚类相匹配。其中,甲基化结果证实(90/104,86.5%)、完善(50/104,48%)或改变(10/104,9.6%)了组织学诊断。只有四项结果被视为无影响(4/104,3.9%)。26 个肿瘤样本的 Cs 值为 0.9。尽管得分较低,但甲基化结果支持了 38.5%(10/26)置信度较低的初步诊断,并确定了两个组织病理学结果不确定的肿瘤的诊断。附加的 t 分布随机邻域嵌入(t-SNE)分析可对 12 个肿瘤进行分类。此外,还有九个样本在使用最新的脑肿瘤分类器后达到了较高的 Cs 值。在希腊共同测试的样本显示出极佳的测试重现性,支持了分析在当地的实施。这项研究支持了将甲基组分析纳入我国常规诊断的必要性,并强调了欧洲儿科肿瘤中心之间合作的重要性。
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The impact of methylome analysis on the diagnosis and treatment of CNS tumours in children and adolescents: A population-based study in Greece

Background

The recently published WHO classification of central nervous system (CNS) tumours recognizes DNA methylation profiling as a desirable and, for some diagnoses, essential diagnostic tool adjunctive to conventional histopathology. DNA methylation profiling is not routinely available in many countries, including Greece.

Methods

In this collaborative study, we report the DNA methylation results in a series of children and adolescents with CNS tumours in Greece (2018–2023). In total, 130 tumour samples were analyzed using the latest applicable version of the Heidelberg brain tumour classifier.

Results

Upon initial analysis, 80 % (104/130) achieved calibrated scores (Cs) ≥ 0.9 and matched an established methylation class family/subclass. Among them, methylation results confirmed (90/104, 86.5 %), refined (50/104, 48 %) or changed (10/104, 9.6 %) the histological diagnosis. Only four results were regarded as non-contributing (4/104, 3.9 %). Twenty-six tumour samples received Cs < 0.9. Despite low scores, methylation results supported the initial diagnosis with lower confidence in 38.5 % (10/26) and established the diagnosis in two tumours with non-conclusive histopathology. Additional t-distributed stochastic neighbour embedding (t-SNE) analysis allowed the possible classification of twelve tumours. Nine more samples reached high Cs using the newer brain tumour classifiers, since available. Samples co-tested in Greece demonstrated excellent test reproducibility, supporting the analysis' local implementation. Methylome profiling impacted the clinical management of 40 % of patients, modifying stratification, prognosis, or treatment approach.

Conclusions

This study supports the need to integrate methylome analysis into routine diagnostics in our country and highlights the importance of collaboration between European pediatric oncology centres.
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