GLIOMA-02 HISTOPATHOLOGIC AND MOLECULAR PROFILE OF GLIOMAS: A 9-YEAR RETROSPECTIVE STUDY OF CASES DIAGNOSED IN LAGOS NIGERIA

IF 3.7 Q1 CLINICAL NEUROLOGY

Neuro-oncology advances Pub Date : 2023-10-31 DOI:10.1093/noajnl/vdad121.002

Lateef Odukoya, Thomas Kollmeyer, Jeanette Eckel-Passow, Cristiane Ida, Daniel Lachance, Ekokobe Fonkem, Kabir Badmos, Olufemi Bankole, Gaspar Kitange, Adetola Daramola, Charles Anunobi, Robert Jenkins

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Abstract

Abstract BACKGROUND The diagnosis and management of patients with brain tumors currently uses WHO defined morphologic and molecular features. However, neuro-oncology practice in low resource settings relies solely on histomorphology. This study aims to reclassify glioma cases diagnosed in the Department of Anatomic and Molecular Pathology Lagos University Teaching Hospital using the WHO 2021 classification. METHODS Fifty-six cases of glioma diagnosed between 2013 to 2021 were evaluated. Morphologic diagnosis was reassessed. Five-micron sections were obtained for immunohistochemistry (IHC), and genetic testing (DNA and RNA) after manual macrodissection for tumor enrichment used 10-µm sections. IHC for IDH1-R132H, ATRX, BRAF-V600E, p53, Ki67 and H3-K27M and Oncoscan chromosomal microarray analysis were performed. NGS mutation/fusion analysis and EPIC methylation array profiling are in progress. RESULTS Of the 56 cases evaluated, median age was 22 years (range, 1-60); 71% were male. The initial morphologic diagnoses included 21 pilocytic astrocytoma, 11 glioblastoma, 9 ependymoma, 7 diffuse astrocytoma, 3 anaplastic astrocytoma, 2 high-grade gliomas, 1 oligodendroglioma, 1 diffuse midline glioma, and 1 pleomorphic xanthoastrocytoma (PXA). Histomorphologic re-evaluation revealed discordant diagnosis in 29% (16/56) of cases. Of the 56 cases, 73% (41/56) had usable DNA yield and 38% (21/56) had DNA yield of ≥750ng. Chromosomal microarray analysis was completed for 50% (28/56) cases. The revised WHO 2021 diagnosis was: 5 glioblastoma IDH-wildtype, 5 pilocytic astrocytoma, 4 glioma NEC, 3 posterior fossa ependymoma, group B, 3 PXA, 3 astrocytoma IDH-mutant, 2 pediatric low-grade gliomas, 2 supratentorial ependymoma, ZFTA fusion-positive, 1 posterior fossa ependymoma, group A. In 71% (20/28) of cases with molecular testing, diagnosis was revised using WHO 2021 criteria. CONCLUSION Most cases had usable DNA. Overall, histologic re-evaluation and molecular based on the WHO 2021 criteria refined the diagnosis in 48% (27/56) of cases.

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胶质瘤的组织病理学和分子特征:尼日利亚拉各斯确诊病例的9年回顾性研究

背景目前脑肿瘤患者的诊断和治疗采用WHO定义的形态学和分子特征。然而，在低资源环境下的神经肿瘤学实践仅依赖于组织形态学。本研究旨在使用世卫组织2021分类对拉各斯大学教学医院解剖和分子病理学部门诊断的胶质瘤病例进行重新分类。方法对2013年至2021年诊断的56例胶质瘤进行评估。重新评估形态学诊断。5微米的切片用于免疫组织化学(IHC)， 10微米的切片用于肿瘤富集的人工宏观解剖后的基因检测(DNA和RNA)。对IDH1-R132H、ATRX、BRAF-V600E、p53、Ki67和H3-K27M进行免疫组化和Oncoscan染色体微阵列分析。NGS突变/融合分析和EPIC甲基化阵列分析正在进行中。结果56例患者中位年龄为22岁(范围1-60岁);71%为男性。初步形态学诊断为毛细胞性星形细胞瘤21例，胶质母细胞瘤11例，室管膜瘤9例，弥漫性星形细胞瘤7例，间变性星形细胞瘤3例，高级别胶质瘤2例，少突胶质细胞瘤1例，弥漫性中线胶质瘤1例，多形性黄色星形细胞瘤1例。组织形态学复查显示29%(16/56)的病例诊断不一致。在56例病例中，73%(41/56)的可用DNA产率，38%(21/56)的DNA产率≥750ng。50%(28/56)病例完成染色体微阵列分析。修订后的WHO 2021诊断为:5例胶质母细胞瘤idh -野生型，5例毛细胞星形细胞瘤，4例胶质瘤NEC, 3例后窝室管膜瘤，B组，3例PXA, 3例星形细胞瘤idh -突变型，2例小儿低级别胶质瘤，2例幕上室管膜瘤，ZFTA融合阳性，1例后窝室管膜瘤，a组。71%(20/28)的分子检测病例，采用WHO 2021标准进行了诊断修订。结论多数病例具有可用DNA。总体而言，基于WHO 2021标准的组织学重新评估和分子诊断改进了48%(27/56)病例的诊断。

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来源期刊

Neuro-oncology advances

CiteScore

6.20

自引率

0.00%

发文量

审稿时长

12 weeks