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MRI-localized biopsies reveal subtype-specific differences in molecular and cellular composition at the margins of glioblastoma

机译:MRI局部活检显示胶质母细胞瘤边缘分子和细胞组成的亚型特异性差异

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摘要

Glioblastomas (GBMs) diffusely infiltrate the brain, making complete removal by surgical resection impossible. The mixture of neoplastic and nonneoplastic cells that remain after surgery form the biological context for adjuvant therapeutic intervention and recurrence. We performed RNA-sequencing (RNA-seq) and histological analysis on radiographically guided biopsies taken from different regions of GBM and showed that the tissue contained within the contrast-enhancing (CE) core of tumors have different cellular and molecular compositions compared with tissue from the nonenhancing (NE) margins of tumors. Comparisons with the The Cancer Genome Atlas dataset showed that the samples from CE regions resembled the proneural, classical, or mesenchymal subtypes of GBM, whereas the samples from the NE regions predominantly resembled the neural subtype. Computational deconvolution of the RNA-seq data revealed that contributions from nonneoplastic brain cells significantly influence the expression pattern in the NE samples. Gene ontology analysis showed that the cell type-specific expression patterns were functionally distinct and highly enriched in genes associated with the corresponding cell phenotypes. Comparing the RNA-seq data from the GBM samples to that of nonneoplastic brain revealed that the differentially expressed genes are distributed across multiple cell types. Notably, the patterns of cell type-specific alterations varied between the different GBM subtypes: the NE regions of proneural tumors were enriched in oligodendrocyte progenitor genes, whereas the NE regions of mesenchymal GBM were enriched in astrocytic and microglial genes. These subtype-specific patterns provide new insights into molecular and cellular composition of the infiltrative margins of GBM.
机译:胶质母细胞瘤(GBMs)弥漫性浸润到大脑中,无法通过手术切除彻底清除。手术后残留的赘生性和非赘生性细胞的混合物形成了辅助治疗干预和复发的生物学环境。我们对来自GBM不同区域的放射线引导的活检组织进行了RNA测序(RNA-seq)和组织学分析,结果显示,与造影剂组织相比,肿瘤的造影剂(CE)核心中包含的组织具有不同的细胞和分子组成肿瘤的非增强(NE)边缘。与癌症基因组图谱数据集的比较显示,CE区的样本类似于GBM的前,亚或间充质亚型,而NE区的样本则主要与神经亚型类似。 RNA-seq数据的计算反卷积显示,非肿瘤性脑细胞的贡献显着影响了NE样品中的表达模式。基因本体分析表明,细胞类型特异性表达模式在功能上是不同的,并且在与相应细胞表型相关的基因中高度富集。将来自GBM样品的RNA-seq数据与非肿瘤性大脑的RNA-seq数据进行比较,发现差异表达的基因分布在多种细胞类型中。值得注意的是,不同GBM亚型之间的细胞类型特异性改变模式有所不同:前突神经瘤的NE区富含少突胶质祖细胞基因,而间充质GBM的NE区富含星形胶质细胞和小胶质细胞基因。这些特定于亚型的模式为GBM浸润边缘的分子和细胞组成提供了新的见识。

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