Targeting the glioblastoma-initiating cell-associated antigens

T. Kondo
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引用次数: 1

Abstract

Glioblastoma (GBM)-initiating cells (GICs) are a tumorigenic subpopulation that are resistant to radio/chemotherapies and are the source of recurrence, therefore it is crucial to characterize GICs and find new therapeutic targets. We have successfully established mouse and human GICs, which retain stemness characteristics and tumorigenicity. By comparing their expression profiles with those of parental cells, we have focused on two cell surface membrane proteins, Ceacam1L and Eva1, which were prominently expressed in GICs. We demonstrated that both proteins were involved in GIC characteristics, including self-renewal, stem cell gene expression and side population, and tumorigenesis, indicating that they are potential new therapeutic targets for GBM. In this research highlight, I summarize our recent reports regarding Ceacam1L and Eva1, and then discuss about Ceacam1L and Eva1 as GBM therapeutic targets.
靶向胶质母细胞瘤起始细胞相关抗原
胶质母细胞瘤(Glioblastoma, GBM)起始细胞(GICs)是一种对放化疗有耐药性的致瘤亚群,是复发的来源,因此对GICs进行表征和寻找新的治疗靶点至关重要。我们已经成功地建立了小鼠和人GICs,它们保留了干性特征和致瘤性。通过比较它们与亲本细胞的表达谱,我们重点关注了两个在gic中显著表达的细胞表面膜蛋白Ceacam1L和Eva1。我们证明这两种蛋白都参与了GIC的特征,包括自我更新、干细胞基因表达和侧群以及肿瘤发生,这表明它们是GBM潜在的新治疗靶点。在本研究重点中,我总结了我们最近关于Ceacam1L和Eva1的报道,然后讨论了Ceacam1L和Eva1作为GBM的治疗靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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