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High-grade gliomas in adolescents and young adults highlight histomolecular differences from their adult and pediatric counterparts

机译:青少年和年轻成年人的高级胶质瘤突出了成人和儿科对应物的组织分子差异

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摘要

Background. Considering that pediatric high-grade gliomas (HGGs) are biologically distinct from their adult counterparts, the objective of this study was to define the landscape of HGGs in adolescents and young adults (AYAs).Methods. We performed a multicentric retrospective study of 112 AYAs from adult and pediatric Ile-de-France neurosurgical units, treated between 1998 and 2013 to analyze their clinicoradiological and histomolecular profiles.The inclusion criteria were age between 15 and 25 years, histopathological HGG diagnosis, available clinical data, and preoperative and follow-up MRI. MRI and tumoral samples were centrally reviewed. Immunohistochemistry and complementary molecular techniques such as targeted/next-generation sequencing, whole exome sequencing, and DNA-methylation analyses were performed to achieve an integrated diagnosis according to the 2016 World Health Organization (WHO) classification.Results. Based on 80 documented AYA patients, HGGs constitute heterogeneous clinicopathological and molecular groups, with a predominant representation of pediatric subtypes (histone H3-mutants, 40%) but also adult subtypes (isocitrate dehydrogenase [IDH] mutants, 28%) characterized by the rarity of oligodendrogliomas, IDH mutants, and 1p/19q codeletion and the relative high frequency of "rare adult IDH mutations" (20%). H3G34-mutants (14%) represent the most specific subgroup in AYAs. In the H3K27-mutant subgroup, non-brainstem diffuse midline gliomas are more frequent (66.7%) than diffuse intrinsic pontine gliomas (23.8%), contrary to what is observed in children. We found that WHO grade has no prognostic value, but molecular subgrouping has major prognostic importance.Conclusions. HGGs in AYAs could benefit from a specific classification, driven by molecular subtyping rather than age group. Collaborative efforts are needed from pediatric and adult neuro-oncology teams to improve the management of HGGs in AYAs.
机译:背景。考虑到儿科高级胶质瘤(HGGS)在其成年人同行中具有生物学上不同的,本研究的目的是定义青少年和年轻成人(Ayas)的HGGS景观。方法。从成人和儿科ILE-法国神经外科单位进行112 AYAS进行多中心回顾性研究,在1998年至2013年间治疗,分析其临床主学和组织分子型材。纳入标准年龄为15至25岁,可用组织病理HGG诊断临床数据,术前和后续MRI。中央审查MRI和肿瘤样品。根据2016年世界卫生组织(WHO)分类,进行免疫组化和互补分子技术,如靶向/下一代测序,全外序测序和DNA-甲基化分析,以实现综合诊断。结果。基于80名记录的AYA患者,HGGS构成异构临床病理和分子基团,其具有小儿亚型的主要表示(组蛋白H3-突变体,40%),但也具有成年亚型(异柠檬酸脱氢酶[IDH]突变体,28%),其特征在于稀有性Oligodendrogliomas,IDH突变体和1P / 19Q Comethion和“稀有成人IDH突变”(20%)的相对高频。 H3G34-突变体(14%)代表Ayas中最具体的亚组。在H3K27-突变体亚组中,非脑干扩散中线胶质瘤比弥漫性内在猪胶质瘤(23.8%)更频繁(66.7%),与儿童观察到的相反。我们发现世卫组织级别没有预后价值,但分子亚组具有重大预后重要性。结论。 Ayas中的HGGS可以受益于特定的分类,由分子亚型而不是年龄组驱动。儿科和成人神经肿瘤学团队需要合作努力,以改善AYAS中HGGS的管理。

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  • 来源
    《Neuro-Oncology》 |2020年第8期|1190-1202|共13页
  • 作者

    Roux Alexandre; Pallud Johan; Saffroy Raphael; Edjlali-Goujon Myriam; Debily Marie-Anne; Boddaert Nathalie; Sanson Marc; Puget Stephanie; Knafo Steven; Adam Clovis; Faillot Thierry; Cazals-Hatem Dominique; Mandonnet Emmanuel; Polivka Marc; Dorfmueller Georges; Dauta Aurelie; Desplanques Mathilde; Gareton Albane; Pages Melanie; Tauziede-Espariat Arnault; Grill Jacques; Bourdeaut Franck; Doz Francois; Dhermain Frederic; Mokhtari Karima; Chretien Fabrice; Figarella-Branger Dominique; Varlet Pascale;

  • 作者单位

    Paris St Anne Hosp Univ Hosp Grp GHU Dept Neurosurg Paris France|Paris Descartes Univ Sorbonne Paris Cite Paris France|Inst Psychiat & Neurosci Paris Imaging Biomarkers Brain Disorders Inserm Unit 1266 Paris France;

    Paris St Anne Hosp Univ Hosp Grp GHU Dept Neurosurg Paris France|Paris Descartes Univ Sorbonne Paris Cite Paris France|Inst Psychiat & Neurosci Paris Imaging Biomarkers Brain Disorders Inserm Unit 1266 Paris France;

    Hop Paul Brousse Dept Biochem Villejuif France;

    Paris Descartes Univ Sorbonne Paris Cite Paris France|Inst Psychiat & Neurosci Paris Imaging Biomarkers Brain Disorders Inserm Unit 1266 Paris France|St Anne Hosp Dept Neuroradiol Paris France;

    Paris Saclay Univ Biomarkers & New Therapeut Targets Oncol Team Genom & Oncogenesis Brain Tumors Paris Sud Univ Inserm Unit 981 Villejuif France|Paris Saclay Univ Evry Univ Evry France;

    Paris Descartes Univ Sorbonne Paris Cite Paris France|Necker Enfants Malad Hosp Dept Neuroradiol Paris France;

    Sorbonne Univ Brain & Spine Inst ICM Expt Neurooncol Dept Inserm U1127 Paris France|Hop La Pitie Salpetriere Dept Neurol 2 Mazarin Unit Paris France;

    Paris Descartes Univ Sorbonne Paris Cite Paris France|Necker Enfants Malad Hosp Dept Neurosurg Paris France;

    Paris Sud Univ Bicetre Hosp Dept Neurosurg Le Kremlin Bicetre France;

    Paris Sud Univ Bicetre Hosp Dept Pathol Le Kremlin Bicetre France;

    Beaujon Hosp Dept Neurosurg Clichy France;

    Beaujon Hosp Dept Pathol Clichy France;

    Lariboisiere Hosp Dept Neurosurg Paris France|Paris 7 Univ Paris France;

    Inst Psychiat & Neurosci Paris Imaging Biomarkers Brain Disorders Inserm Unit 1266 Paris France|Lariboisiere Hosp Dept Pathol Paris France;

    Rothschild Fdn Hosp Dept Pediat Neurosurg Paris France;

    Henri Mordor Hosp Dept Neurosurg Creteil France;

    GHU Paris St Anne Hosp Dept Neuropathol Paris France;

    Paris Descartes Univ Sorbonne Paris Cite Paris France;

    Paris Descartes Univ Sorbonne Paris Cite Paris France;

    Paris Descartes Univ Sorbonne Paris Cite Paris France|Inst Psychiat & Neurosci Paris Imaging Biomarkers Brain Disorders Inserm Unit 1266 Paris France;

    Paris Saclay Univ Biomarkers & New Therapeut Targets Oncol Team Genom & Oncogenesis Brain Tumors Paris Sud Univ Inserm Unit 981 Villejuif France|Paris Saclay Univ Paris Sud Univ Gustave Roussy Univ Hosp Dept Pediat Oncol Villejuif France;

    Paris Descartes Univ Sorbonne Paris Cite Paris France|Inst Curie SIREDO Oncol Ctr Care Innovat & Res Children & AY Paris France;

    Paris Descartes Univ Sorbonne Paris Cite Paris France|Inst Curie SIREDO Oncol Ctr Care Innovat & Res Children & AY Paris France;

    Gustave Roussy Univ Hosp Dept Radiotherapy Villejuif France;

    Necker Enfants Malad Hosp Dept Neuroradiol Paris France|Hop La Pitie Salpetriere Dept Neuropathol Paris France;

    Gustave Roussy Univ Hosp Dept Radiotherapy Villejuif France;

    Timone Hosp Dept Pathol & Neuropathol Marseille France;

    Paris Descartes Univ Sorbonne Paris Cite Paris France|Inst Psychiat & Neurosci Paris Imaging Biomarkers Brain Disorders Inserm Unit 1266 Paris France;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    DNA-methylation analysis; glioblastoma; glioma; integrated diagnosis; whole exome sequencing;

    机译:DNA-甲基化分析;胶质母细胞瘤;胶质瘤;综合诊断;整体exame测序;
  • 入库时间 2022-08-18 23:31:58

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