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侵袭性中枢神经细胞瘤的肿瘤球具有增强的表皮生长因子受体和肿瘤干细胞信号传导的过渡扩增祖细胞特征。

Tumor Spheroids of an Aggressive Form of Central Neurocytoma Have Transit-Amplifying Progenitor Characteristics with Enhanced EGFR and Tumor Stem Cell Signaling.

作者信息

Shin Hye Young, Han Kyung-Seok, Park Hyung Woo, Hong Yun Hwa, Kim Yona, Moon Hyo Eun, Park Kwang Woo, Park Hye Ran, Lee C Justin, Lee Kiyoung, Kim Sang Jeong, Heo Man Seung, Park Sung-Hye, Kim Dong Gyu, Paek Sun Ha

机构信息

Department of Neurosurgery, Seoul National University College of Medicine, Seoul 03082, Korea.

Center for Cognition and Sociality, Institute for Basic Science, Daejeon 34126, Korea.

出版信息

Exp Neurobiol. 2021 Apr 30;30(2):120-143. doi: 10.5607/en21004.

Abstract

Central neurocytoma (CN) has been known as a benign neuronal tumor. In rare cases, CN undergoes malignant transformation to glioblastomas (GBM). Here we examined its cellular origin by characterizing differentiation potential and gene expression of CN-spheroids. First, we demonstrate that both CN tissue and cultured primary cells recapitulate the hierarchal cellular composition of subventricular zone (SVZ), which is comprised of neural stem cells (NSCs), transit amplifying progenitors (TAPs), and neuroblasts. We then derived spheroids from CN which displayed EGFR+/ MASH+ TAP and BLBP+ radial glial cell (RGC) characteristic, and mitotic neurogenesis and gliogenesis by single spheroids were observed with cycling multipotential cells. CN-spheroids expressed increased levels of pluripotency and tumor stem cell genes such as and , when compared to their differentiated cells and human NSCs. Importantly, Gene Set Enrichment Analysis showed that gene sets of GBM-Spheroids, EGFR Signaling, and Packaging of Telomere Ends are enriched in CN-spheroids in comparison with their differentiated cells. We speculate that CN tumor stem cells have TAP and RGC characteristics, and upregulation of EGFR signaling as well as downregulation of eph-ephrin signaling have critical roles in tumorigenesis of CN. And their ephemeral nature of TAPs destined to neuroblasts, might reflect benign nature of CN.

摘要

中枢神经细胞瘤(CN)一直被认为是一种良性神经元肿瘤。在罕见情况下,CN会恶变为胶质母细胞瘤(GBM)。在此,我们通过表征CN球状体的分化潜能和基因表达来研究其细胞起源。首先,我们证明CN组织和培养的原代细胞都重现了脑室下区(SVZ)的分层细胞组成,该区域由神经干细胞(NSCs)、过渡扩增祖细胞(TAPs)和成神经细胞组成。然后,我们从CN中获得了球状体,这些球状体表现出EGFR+/MASH+ TAP和BLBP+放射状胶质细胞(RGC)特征,并且通过循环多能细胞观察到单个球状体的有丝分裂神经发生和胶质发生。与它们的分化细胞和人类神经干细胞相比,CN球状体中多能性和肿瘤干细胞基因如 和 的表达水平升高。重要的是,基因集富集分析表明,与它们的分化细胞相比,GBM球状体、EGFR信号和端粒末端包装的基因集在CN球状体中富集。我们推测,CN肿瘤干细胞具有TAP和RGC特征,EGFR信号的上调以及eph-ephrin信号的下调在CN的肿瘤发生中起关键作用。并且它们向成神经细胞定向的TAPs的短暂性质,可能反映了CN的良性性质。

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