Glioma tropic neural stem cells consist of astrocytic precursors and their migratory capacity is mediated by CXCR4.

Moneeb Ehtesham, Xiangpeng Yuan, Peter Kabos, Nancy H C Chung, Gentao Liu, Yasuharu Akasaki, Keith L Black, John S Yu
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引用次数: 162

Abstract

Malignant gliomas spawn disseminated microsatellites, which are largely refractory to currently employed therapies, resulting in eventual tumor recurrence and death. The use of tumor-tropic neural stem cells (NSCs) as delivery vehicles for therapeutic gene products represents an attractive strategy specifically focused at treating these residual neoplastic foci. We wished to elucidate the biological cues governing NSC tropism for glioma. In this context, we describe that tumor-tropic NSCs comprise largely of astrocytic progenitors expressing chemokine receptor 4 (CXCR4). Blocking of CXCR4 significantly inhibits NSC migration toward the tumor. These findings define specific characteristics associated with the cell populations within transplanted NSCs that demonstrate glioma-tracking behavior.

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嗜胶质瘤神经干细胞由星形细胞前体组成,其迁移能力由CXCR4介导。
恶性胶质瘤产生弥散性微卫星,目前使用的治疗方法在很大程度上是难治的,最终导致肿瘤复发和死亡。使用致瘤性神经干细胞(NSCs)作为治疗性基因产品的递送载体,是一种有吸引力的策略,专门用于治疗这些残留的肿瘤病灶。我们希望阐明控制NSC对胶质瘤的偏向性的生物学线索。在这种情况下,我们描述了致瘤性NSCs主要由表达趋化因子受体4 (CXCR4)的星形细胞祖细胞组成。阻断CXCR4可显著抑制NSC向肿瘤的迁移。这些发现定义了移植的NSCs中与胶质瘤跟踪行为相关的细胞群的特定特征。
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