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CD133/CD15 定义了具有不同体外克隆活性和与干细胞相关基因表达谱的不同细胞亚群,这些细胞亚群来自具有 PNET 样成分的体外增殖多形性成胶质细胞瘤源性细胞系。

CD133/CD15 defines distinct cell subpopulations with differential in vitro clonogenic activity and stem cell-related gene expression profile in in vitro propagated glioblastoma multiforme-derived cell line with a PNET-like component.

机构信息

Division of Stereotactic Neurosurgery, Department of General Neurosurgery, University Medical Center Freiburg, Freiburg, Germany.

出版信息

Folia Neuropathol. 2012;50(4):357-68. doi: 10.5114/fn.2012.32365.

Abstract

Glioblastoma multiforme (GBM), as many other solid tumours, contains a subpopulation of cells termed cancer stem-like cells responsible for the initiation and propagation of tumour growth. However, a unique immunophenotype/surface antigen composition for the clear identification of brain tumour stem cells (BTSC) has not yet been found. Here we report a novel code of cell surface markers for the identification of different cell subpopulations in neurospheres derived from a GBM with a primitive neuroectodermal tumour (PNET)-like component (GBM-PNET). These subgroups differ in their CD133/CD15 expression pattern and resemble cells with different stem-like genotype and developmental pathway activation levels. Strikingly, clonogenic analysis of cultures differentially expressing the investigated markers enabled the identification of distinct subpopulations of cells endowed with stem cell characteristics. High clonogenicity could be found in CD133(-)/CD15(-) and CD133(+)/CD15(+) but not in CD133(-)/CD15(+) cells. Moreover, cell subpopulations with pronounced clonogenic growth were characterized by high expression of stem cell-related genes. Interestingly, these observations were unique for GBM-PNET and differed from ordinary GBM cultures derived from tumours lacking a PNET component. This work elucidates the complex molecular heterogeneity of in vitro propagated glioblastoma-derived cells and potentially contributes to the development of novel diagnostic modalities aiming at the identification of the brain tumour stem-like cell population in a subgroup of GBMs.

摘要

多形性胶质母细胞瘤(GBM)与许多其他实体瘤一样,含有一小部分被称为癌症干细胞样细胞的细胞,这些细胞负责肿瘤生长的起始和增殖。然而,目前尚未发现用于明确鉴定脑肿瘤干细胞(BTSC)的独特免疫表型/表面抗原组成。在这里,我们报告了一种新的细胞表面标志物代码,用于鉴定源自具有原始神经外胚层肿瘤(PNET)样成分的 GBM(GBM-PNET)的神经球中不同的细胞亚群。这些亚群在 CD133/CD15 表达模式上存在差异,类似于具有不同干细胞样基因型和发育途径激活水平的细胞。引人注目的是,对差异表达研究标志物的培养物进行克隆分析,能够鉴定具有干细胞特征的不同细胞亚群。在 CD133(-)/CD15(-)和 CD133(+)/CD15(+)细胞中可以发现高克隆形成能力,但在 CD133(-)/CD15(+)细胞中则不然。此外,具有明显克隆生长能力的细胞亚群表现出高水平的与干细胞相关的基因表达。有趣的是,这些观察结果是 GBM-PNET 所特有的,与缺乏 PNET 成分的普通 GBM 培养物不同。这项工作阐明了体外增殖的胶质母细胞瘤衍生细胞的复杂分子异质性,并可能有助于开发新的诊断方法,旨在鉴定一组 GBM 中的脑肿瘤干细胞样细胞群体。

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