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Molecular diagnostic testing of diffuse gliomas in the real-life setting: A practical approach

机译:实际环境中扩散胶质瘤的分子诊断测试:一种实用的方法

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摘要

Typing of diffuse gliomas according to the WHO 2016 Classification of Tumors of the Central Nervous System is based on the integration of histology with molecular biomarkers. However, the choice of appropriate methods for molecular analysis and criteria for interpretation of test results is left to each diagnostic laboratory. In the present study, we tested the applicability of combined immunohistochemistry, direct sequencing, and multiplex ligation-dependent probe amplification (MLPA) for diagnostic assessment of IDH1/2 mutation status, chromosome 1p/19q status, and TERT promoter mutations. To this end, we analyzed a consecutive series of 165 patients with diffuse low- and high-grade gliomas (WHO grade II and III) from three Austrian centers in which tissue specimens were routinely processed. We could reliably detect IDH1/2 mutations by combining immunohistochemistry, direct sequencing, and MLPA analysis. MLPA analysis also allowed reliable detection of combined whole chromosomal arm 1p/19q codeletion when using carefully selected criteria providing an optimal balance between sensitivity and specificity. Direct sequencing proved to be suitable for identification of TERT promoter mutations, although its analytical performance remains to be assessed. To conclude, we propose a practicable combination of methods and criteria which allow reliable molecular diagnostic testing of diffuse gliomas in the real-life setting.
机译:根据中枢神经系统肿瘤的世卫组织分类,衍射弥漫性胶质瘤是基于组织学与分子生物标志物的整合。然而,对每个诊断实验室留给每个诊断实验室的分子分析和解释标准的适当方法。在本研究中,我们测试了用于诊断评估IDH1 / 2突变状态,染色体1P / 19Q状态和TERT启动子突变的组合免疫组织化学,直接测序和多重连接依赖性探针扩增(MLPA)的适用性。为此,我们分析了来自三个奥地利中心的弥漫性低级和高级胶质瘤(世卫组织二级和III)的连续系列,其中包括组织标本的常规处理。通过组合免疫组织化学,直接测序和MLPA分析,我们可以可靠地检测IDH1 / 2突变。当使用仔细选择的标准时,MLPA分析还允许在敏感性和特异性之间提供最佳平衡时可靠地检测组合的整个染色体臂1P / 19Q Comeplion。证明是适合于鉴定TERT启动子突变的直接测序,尽管其分析性能仍有待评估。为了得出结论,我们提出了一种可行的方法和标准组合,其允许可靠的分子诊断测试在现实生活中的弥漫性胶质瘤。

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