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Glioma Stem Cells and Their Microenvironments: Providers of Challenging Therapeutic Targets

机译:胶质瘤干细胞及其微环境:挑战治疗目标的提供者

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摘要

Malignant gliomas are aggressive brain tumors with limited therapeutic options, possibly because of highly tumorigenic subpopulations of glioma stem cells. These cells require specific microenvironments to maintain their "stemness," described as perivascular and hypoxic niches. Each of those niches induces particular signatures in glioma stem cells (e.g., activation of Notch signaling, secretion of VEGF, bFGF, SDF1 for the vascular niche, activation of HIF2 alpha, and metabolic reprogramming for hypoxic niche). Recently, accumulated knowledge on tumor-associated macrophages, possibly delineating a third niche, has underlined the role of immune cells in glioma progression, via specific chemoattractant factors and cytokines, such as macrophage-colony stimulation factor (M-CSF). The local or myeloid origin of this new component of glioma stem cells niche is yet to be determined. Such niches are being increasingly recognized as key regulators involved in multiple stages of disease progression, therapy resistance, immune-escaping, and distant metastasis, thereby substantially impacting the future development of frontline interventions in clinical oncology. This review focuses on the microenvironment impact on the glioma stem cell biology, emphasizing GSCs cross talk with hypoxic, perivascular, and immune niches and their potential use as targeted therapy.
机译:恶性胶质瘤是具有有限治疗选择的侵袭性脑肿瘤,可能是因为胶质瘤干细胞的高度致致瘤族群。这些细胞需要特异性微环境以保持其“茎干”,描述为血管外和缺氧效力。这些核桃中的每一个在胶质瘤干细胞中诱导特定签名(例如,缺口信号传导,VEGF的分泌,BFGF,SDF1的血管利基,HIF2α的激活,以及对缺氧NICHE的代谢重编程)。最近,累积对肿瘤相关巨噬细胞的知识,可能描绘第三个乳蛋白,通过特异性化学趋然因子和细胞因子(例如巨噬细胞殖民刺激因子(M-CSF),强调了免疫细胞在胶质瘤进展中的作用。这种新组分的胶质瘤干细胞Niche的局部或骨髓起源尚未确定。这种效力越来越被认为是涉及疾病进展,治疗抵抗,免疫逃逸和远端转移的多个阶段的关键调节因子,从而显着影响临床肿瘤学中的前线干预的未来发展。本综述重点介绍对胶质瘤干细胞生物学的微环境影响,强调GSCS与缺氧,血管外和免疫力伴侣及其潜在用途作为靶向治疗。

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