首页> 外文期刊>Stem cells and development >Persistence of CD133+ cells in human and mouse glioma cell lines: detailed characterization of GL261 glioma cells with cancer stem cell-like properties.
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Persistence of CD133+ cells in human and mouse glioma cell lines: detailed characterization of GL261 glioma cells with cancer stem cell-like properties.

机译:人和小鼠神经胶质瘤细胞系中CD133 +细胞的持久性:具有癌症干细胞样特性的GL261神经胶质瘤细胞的详细表征。

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The concept of cancer stem cells suggests that there are malignant stem-like cells within a tumor that are responsible for tumor renewal and resistance to cytotoxic therapies. Studies have identified glioma stem-like cells that extrude Hoechst 33342 dye, representing a double-negative "side population" (SP) thought to be selectively resistant to drug therapy. A CD133+ stem cell-like subpopulation has been isolated from a human glioma that was enriched for tumor-initiating cells. It is unknown whether CD133+ cells with similar phenotype persist in established glioma cell lines, or if CD133 is a marker of glioma stem-like cells in rodents. We investigated whether CD133+ and SP cells existed in the GL261 cell line, a syngeneic mouse glioma model that is widely used for preclinical and translational research. Intracerebral injection of less than 100 CD133+ GL261 cells formed tumors, whereas it required 10,000 CD133(-) cells to initiate a tumor. CD133+ GL261 cells expressed nestin, formed tumor spheres withhigh frequency, and differentiated into glial and neuronal-like cells. Similar to GL261, seven human glioma cell lines analyzed also contained a rare CD133+ population. Surprisingly, we found that CD133+ GL261 cells did not reside in the SP, nor did the majority ( approximately 94%) of CD133+ human glioma cells. These results demonstrate that the expression of CD133 in murine glioma cells is associated with enhanced tumorigenicity and a stem-like phenotype. This study also reveals a previously unrecognized level of heterogeneity in glioma cell lines, exposing several populations of cells that have characteristics of cancer stem cells.
机译:癌症干细胞的概念表明,肿瘤内有恶性干样细胞,负责肿瘤的更新和对细胞毒性疗法的抵抗力。研究已经确定,神经胶质瘤干细胞可以挤出Hoechst 33342染料,代表被认为对药物治疗有选择性抵抗的双阴性“侧群”(SP)。已经从富含神经胶质瘤的人的神经胶质瘤中分离出了CD133 +干细胞样亚群。目前尚不清楚表型相似的CD133 +细胞是否仍存在于已建立的神经胶质瘤细胞系中,或者CD133是啮齿动物中神经胶质瘤干细胞样细胞的标志物。我们研究了GL261细胞系中是否存在CD133 +和SP细胞,GL261细胞系是一种同基因小鼠神经胶质瘤模型,广泛用于临床前和翻译研究。脑内注射少于100个CD133 + GL261细胞会形成肿瘤,而需要10,000个CD133(-)细胞才能引发肿瘤。 CD133 + GL261细胞表达巢蛋白,高频率形成肿瘤球,并分化为神经胶质细胞和神经元样细胞。与GL261相似,分析的7种人类神经胶质瘤细胞系也含有罕见的CD133 +群体。令人惊讶的是,我们发现CD133 + GL261细胞既不存在于SP中,也不存在大部分(约94%)CD133 +人神经胶质瘤细胞。这些结果表明,CD133在鼠神经胶质瘤细胞中的表达与致瘤性增强和茎样表型有关。这项研究还揭示了胶质瘤细胞系中以前无法识别的异质性水平,暴露了具有癌症干细胞特征的几种细胞群。

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