首页> 美国卫生研究院文献>Neuro-Oncology >EPEN-12. A COMMON FETAL DEVELOPMENTAL ORIGIN FOR PFA EPENDYMOMA PFB EPENDYMOMA AND CEREBELLAR PILOCYTIC ASTROCYTOMAS
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EPEN-12. A COMMON FETAL DEVELOPMENTAL ORIGIN FOR PFA EPENDYMOMA PFB EPENDYMOMA AND CEREBELLAR PILOCYTIC ASTROCYTOMAS

机译:EPEN-12。 PFA表皮瘤PFB表皮瘤和小脑上皮星形胶质细胞瘤的共同胎儿发育起源

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摘要

Single cell RNA-sequencing (scRNAseq) of the murine cerebellum at nine fetal and immediate post-natal (E10-P14) times points on >60,000 individual cells to identified >30 transcriptionally distinct cell clusters. Based on marker gene expression, many clusters resemble known cerebellar stem, progenitor, and differentiated cell types, while other clusters are more novel. Pseudo-time trajectory assisted in the reconstruction of known and novel developmental lineages, including the lineage of the cerebellar radial glia. A population of stem cells in the ventricular zone (VZ) gives rise to the progenitors of the GABAergic cerebellar interneurons, as well as the gliogenic progenitor cells, which subsequently become Bergmann glia and astrocytes. A novel, but clearly distinct and robust cluster of cells with transcriptional similarity to both the roof plate and the rhombic lip was identified. Comparison of bulk RNA-seq from human PFA, PFB, and cerebellar pilocytic astrocytomas (C-PA) reveals that all three-tumor types best transcriptionally match the gliogenic progenitor cells, with some similarity to VZ progenitor cells and ‘roof plate like’ stem cells. Furthermore, PFA and PFB temporally match to the gliogenic progenitors at E16, while C-PA resemble the E16-E18 the progenitor population. Subclustering of gliogenic progenitors reveals significant intra-cluster heterogeneity, with the ependymomas transcriptionally matching one subcluster, and the C-PA clearly matching a very different subcluster. scRNAseq of human PFA and C-PA reveals multiple tumor cell clusters within a given human ependymoma, with some clusters matching most closely to the gliogenic progenitors, and others matching best to the ‘roof plate like’ stem cells. Similarity to the ‘roof plate stem cells’ (E10-E14), and gliogenic progenitors (E14-E18) suggests an embryonic origin for PFA, PFB, and C-PA, suggests specific novel cells of origin, and offers a novel opportunity to understand posterior fossa tumor transcriptomic targets for novel therapy.
机译:在9个胎儿和出生后即刻(E10-P14)时间,鼠小脑的单细胞RNA测序(scRNAseq)指向> 60,000个单个细胞,从而鉴定出> 30个转录不同的细胞簇。基于标记基因的表达,许多簇类似于已知的小脑干,祖细胞和分化的细胞类型,而其他簇则更为新颖。伪时间轨迹有助于重建已知和新颖的发育谱系,包括小脑radial神经胶质谱系。在心室区(VZ)中的干细胞群体产生了GABA能小脑中间神经元的祖细胞以及胶质生成祖细胞,后者随后变成了Bergmann胶质细胞和星形胶质细胞。鉴定出新颖的,但明显不同且健壮的细胞簇,其与屋顶板和菱形唇的转录相似。人类PFA,PFB和小脑毛细胞星形细胞瘤(C-PA)的大量RNA-seq的比较显示,所有三肿瘤类型在转录上均与胶质生成祖细胞最匹配,与VZ祖细胞和“屋顶板状”茎有些相似细胞。此外,PFA和PFB在时间上与E16的胶质生成祖细胞相匹配,而C-PA与E16-E18的祖细胞相似。胶质生成祖细胞的亚簇揭示了显着的簇内异质性,室管膜瘤在转录上与一个亚簇匹配,而C-PA明显与一个非常不同的亚簇匹配。人类PFA和C-PA的scRNAseq显示在给定的人类室管膜瘤中有多个肿瘤细胞簇,其中一些簇与胶质细胞祖细胞最接近,而其他簇与“屋顶板状”干细胞最匹配。与“屋顶板干细胞”(E10-E14)和胶质生成祖细胞(E14-E18)相似,表明PFA,PFB和C-PA的胚胎起源,暗示了特定的新型起源细胞,并提供了新的机会了解后颅窝肿瘤转录组靶点的新疗法。

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