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弥漫性中线胶质瘤,H3 K27M 突变的转录组和表观遗传分析根据突变的组蛋白 H3 的类型而不是幕上或幕下位置对两个亚组进行区分。

Transcriptomic and epigenetic profiling of 'diffuse midline gliomas, H3 K27M-mutant' discriminate two subgroups based on the type of histone H3 mutated and not supratentorial or infratentorial location.

机构信息

UMR8203,Vectorologie et Nouvelles Thérapies Anticancéreuses, CNRS, Gustave Roussy, Univ. Paris-Sud, Université Paris-Saclay, 94805, Villejuif, France.

Département de Cancérologie de l'Enfant et de l'Adolescent, Institut de Cancérologie Gustave Roussy, Université Paris-Sud, Université Paris-Saclay, 114 rue Édouard Vaillant, 94805, Villejuif Cedex, France.

出版信息

Acta Neuropathol Commun. 2018 Nov 5;6(1):117. doi: 10.1186/s40478-018-0614-1.

Abstract

Diffuse midline glioma (DMG), H3 K27M-mutant, is a new entity in the updated WHO classification grouping together diffuse intrinsic pontine gliomas and infiltrating glial neoplasms of the midline harboring the same canonical mutation at the Lysine 27 of the histones H3 tail.Two hundred and fifteen patients younger than 18 years old with centrally-reviewed pediatric high-grade gliomas (pHGG) were included in this study. Comprehensive transcriptomic (n = 140) and methylation (n = 80) profiling was performed depending on the material available, in order to assess the biological uniqueness of this new entity compared to other midline and hemispheric pHGG.Tumor classification based on gene expression (GE) data highlighted the similarity of K27M DMG independently of their location along the midline. T-distributed Stochastic Neighbor Embedding (tSNE) analysis of methylation profiling confirms the discrimination of DMG from other well defined supratentorial tumor subgroups. Patients with diffuse intrinsic pontine gliomas (DIPG) and thalamic DMG exhibited a similarly poor prognosis (11.1 and 10.8 months median overall survival, respectively). Interestingly, H3.1-K27M and H3.3-K27M primary tumor samples could be distinguished based both on their GE and DNA methylation profiles, suggesting that they might arise from a different precursor or from a different epigenetic reorganization.These differences in DNA methylation profiles were conserved in glioma stem-like cell culture models of DIPG which mimicked their corresponding primary tumor. ChIP-seq profiling of H3K27me3 in these models indicate that H3.3-K27M mutated DIPG stem cells exhibit higher levels of H3K27 trimethylation which are correlated with fewer genes expressed by RNAseq. When considering the global distribution of the H3K27me3 mark, we observed that intergenic regions were more trimethylated in the H3.3-K27M mutated cells compared to the H3.1-K27M mutated ones.H3 K27M-mutant DMG represent a homogenous group of neoplasms compared to other pediatric gliomas that could be further separated based on the type of histone H3 variant mutated and their respective epigenetic landscapes. As these characteristics drive different phenotypes, these findings may have important implication for the design of future trials in these specific types of neoplasms.

摘要

弥漫性中线胶质瘤(DMG),H3 K27M 突变型,是更新后的世界卫生组织分类中的一个新实体,将弥漫性内在脑桥胶质瘤和中线浸润性神经胶质瘤聚集在一起,这些肿瘤均携带组蛋白 H3 尾部赖氨酸 27 位的相同经典突变。本研究纳入了 215 名年龄小于 18 岁的经中心审查的小儿高级别胶质瘤(pHGG)患者。根据可用材料进行了综合转录组(n=140)和甲基化(n=80)分析,以评估与其他中线和大脑半球 pHGG 相比,这种新实体的生物学独特性。基于基因表达(GE)数据的肿瘤分类突出了 K27M DMG 的相似性,而与它们在中线的位置无关。甲基化分析的 t 分布随机邻域嵌入(tSNE)分析证实了 DMG 与其他明确定义的幕上肿瘤亚组的区分。弥漫性内在脑桥胶质瘤(DIPG)和丘脑 DMG 患者的总生存中位数分别为 11.1 和 10.8 个月,预后相似。有趣的是,H3.1-K27M 和 H3.3-K27M 原发性肿瘤样本可基于其 GE 和 DNA 甲基化谱进行区分,表明它们可能来自不同的前体细胞或不同的表观遗传重排。这些 DNA 甲基化谱的差异在 DIPG 神经干细胞的胶质瘤干细胞样培养模型中得到了保留,这些模型模拟了相应的原发性肿瘤。这些模型中 H3K27me3 的 ChIP-seq 分析表明,H3.3-K27M 突变的 DIPG 干细胞表现出更高水平的 H3K27 三甲基化,这与 RNAseq 表达的基因较少相关。当考虑 H3K27me3 标记的全局分布时,我们观察到与 H3.1-K27M 突变细胞相比,基因间区域在 H3.3-K27M 突变细胞中被更多地三甲基化。与其他小儿胶质瘤相比,H3 K27M 突变型 DMG 是一组同质的肿瘤,可进一步根据突变的组蛋白 H3 变体类型及其各自的表观遗传景观进行区分。由于这些特征驱动不同的表型,这些发现可能对这些特定类型肿瘤的未来试验设计具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/82df/6219253/63962c7d67ab/40478_2018_614_Fig1_HTML.jpg

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