趋化因子 CXC 受体 4 介导的骨髓源性神经祖细胞/干细胞对脑肿瘤的跟踪。
Chemokine CXC receptor 4--mediated glioma tumor tracking by bone marrow--derived neural progenitor/stem cells.
机构信息
Department of Neurosurgery, Cedars-Sinai Medical Center, Los Angeles, California, USA.
出版信息
Mol Cancer Ther. 2009 Sep;8(9):2746-53. doi: 10.1158/1535-7163.MCT-09-0273. Epub 2009 Sep 1.
Malignant gliomas manifest frequent tumor recurrence after surgical resection and/or other treatment because of their nature of invasiveness and dissemination. The recognized brain tumor-tracking property of neural progenitor/stem cells opened the possibility of targeting malignant brain tumors using neural progenitor/stem cells. We and others have previously shown that fetal neural progenitor/stem cells can be used to deliver therapeutic molecules to brain tumors. Our recent work has further shown that gene delivery by bone marrow-derived neural progenitor/stem cells achieves therapeutic effects in a glioma model. In this study, we isolate and characterize bone marrow-derived neural progenitor/stem cells, which also express the chemokine receptor chemokine CXC receptor 4 (CXCR4). We show that CXCR4 is required for their chemotaxis and extracellular matrix invasion against a gradient of glioma soluble factors. Furthermore, beta-galactosidase-labeled bone marrow-derived neural progenitor/stem cells implanted in the contralateral side of the brain were shown to track gliomas as early as day 1 and increased through days 3 and 7. Intracranial glioma tracking by bone marrow-derived neural progenitor/stem cells is significantly inhibited by preincubation of bone marrow-derived neural progenitor/stem cells with a blocking anti-CXCR4 antibody, suggesting a CXCR4-dependent tracking mechanism. Glioma tracking bone marrow-derived neural progenitor/stem cells were found to express progenitor/stem cell markers, as well as CXCR4. Although bromodeoxyuridine incorporation assays and proliferating antigen staining indicated that tumor tracking bone marrow-derived neural progenitor/stem cells were mostly nonproliferating, these cells survive in the local tumor environment with little apoptosis. Elucidating the molecular mechanism of brain tumor tracking by adult source stem cells may provide basis for the development of future targeted therapy for malignant brain tumors.
恶性神经胶质瘤由于其侵袭性和扩散性,在手术切除和/或其他治疗后经常复发。神经祖细胞/干细胞对脑肿瘤的识别特性为利用神经祖细胞/干细胞靶向恶性脑肿瘤提供了可能。我们和其他人以前已经表明,胎儿神经祖细胞/干细胞可以用于向脑肿瘤递送治疗分子。我们最近的工作进一步表明,骨髓源性神经祖细胞/干细胞的基因传递在神经胶质瘤模型中实现了治疗效果。在这项研究中,我们分离并鉴定了骨髓源性神经祖细胞/干细胞,它们也表达趋化因子受体趋化因子 CXC 受体 4(CXCR4)。我们表明,CXCR4 是其趋化性和细胞外基质对神经胶质瘤可溶性因子梯度的侵袭所必需的。此外,植入大脑对侧的β-半乳糖苷酶标记的骨髓源性神经祖细胞/干细胞在第 1 天就已经开始追踪神经胶质瘤,并在第 3 天和第 7 天增加。用阻断性抗 CXCR4 抗体预先孵育骨髓源性神经祖细胞/干细胞,显著抑制了骨髓源性神经祖细胞/干细胞对颅内神经胶质瘤的追踪,这表明存在一种依赖于 CXCR4 的追踪机制。发现追踪神经胶质瘤的骨髓源性神经祖细胞/干细胞表达祖细胞/干细胞标志物以及 CXCR4。尽管溴脱氧尿苷掺入测定和增殖抗原染色表明,肿瘤追踪骨髓源性神经祖细胞/干细胞大多不增殖,但这些细胞在局部肿瘤环境中生存,凋亡很少。阐明成体来源干细胞对脑肿瘤的追踪的分子机制可能为恶性脑肿瘤的靶向治疗的发展提供基础。
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