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Update on the integrated histopathological and genetic classification of medulloblastoma – a practical diagnostic guideline

机译:髓母细胞瘤组织病理学和遗传学综合分类的最新进展-实用的诊断指南

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摘要

The revised WHO classification of tumors of the CNS 2016 has introduced the concept of the integrated diagnosis. The definition of medulloblastoma entities now requires a combination of the traditional histological information with additional molecular/genetic features. For definition of the histopathological component of the medulloblastoma diagnosis, the tumors should be assigned to one of the four entities classic, desmoplasticodular (DNMB), extensive nodular (MBEN), or large cell/anaplastic (LC/A) medulloblastoma. The genetically defined component comprises the four entities WNT-activated, SHH-activated and TP53 wildtype, SHH-activated and TP53 mutant, or non-WNTon-SHH medulloblastoma. Robust and validated methods are available to allow a precise diagnosis of these medulloblastoma entities according to the updated WHO classification, and for differential diagnostic purposes. A combination of immunohistochemical markers including β-catenin, Yap1, p75-NGFR, Otx2, and p53, in combination with targeted sequencing and copy number assessment such as FISH analysis for MYC genes allows a precise assignment of patients for risk-adapted stratification. It also allows comparison to results of study cohorts in the past and provides a robust basis for further treatment refinement.
机译:修订后的CNS 2016的WHO肿瘤分类引入了综合诊断的概念。髓母细胞瘤实体的定义现在需要结合传统的组织学信息和其他分子/遗传学特征。为了定义髓母细胞瘤诊断的组织病理学成分,应将肿瘤分配为经典的四个实体之一,即:增生/结节性(DNMB),广泛性结节性(MBEN)或大细胞/间变性(LC / A)髓母细胞瘤。遗传定义的成分包括四个实体:WNT激活,SHH激活和TP53野生型,SHH激活和TP53突变或非WNT /非SHH髓母细胞瘤。现有可靠且经过验证的方法可根据更新的WHO分类对这些髓母细胞瘤实体进行精确诊断,并用于鉴别诊断。免疫组织化学标记物(包括β-连环蛋白,Yap1,p75-NGFR,Otx2和p53)与靶向测序和拷贝数评估(例如MYC基因的FISH分析)相结合,可以精确地分配患者以进行风险适应性分层。它也可以与过去的研究结果进行比较,并为进一步改善治疗方法提供了坚实的基础。

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