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Understanding cytoskeleton regulators in glioblastoma multiforme for therapy design

机译:了解胶质母细胞瘤中的细胞骨架调节剂以进行治疗设计

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摘要

The cellular cytoskeleton forms the primary basis through which a cell governs the changes in size, shape, migration, proliferation, and forms the primary means through which the cells respond to their environment. Indeed, cell and tissue morphologies are used routinely not only to grade tumors but also in various high-content screening methods with an aim to identify new small molecules with therapeutic potential. This study examines the expression of various cytoskeleton regulators in glioblastoma multiforme (GBM). GBM is a very aggressive disease with a low life expectancy even after chemo- and radiotherapy. Cancer cells of GBM are notorious for their invasiveness, ability to develop resistance to chemo- and radiotherapy, and to form secondary site tumors. This study aims to gain insight into cytoskeleton regulators in GBM cells and to understand the effect of various oncology drugs, including temozolomide, on cytoskeleton regulators. We compare the expression of various cytoskeleton regulators in GBM-derived tumor and normal tissue, CD133-postive and -negative cells from GBM and neural cells, and GBM stem-like and differentiated cells. In addition, the correlation between the expression of cytoskeleton regulators with the clinical outcome was examined to identify genes associated with longer patient survival. This was followed by a small molecule screening with US Food and Drug Administration (FDA)-approved oncology drugs, and its effect on cellular cytoskeleton was compared to treatment with temozolomide. This study identifies various groups of cytoskeletal regulators that have an important effect on patient survival and tumor development. Importantly, this work highlights the advantage of using cytoskeleton regulators as biomarkers for assessing prognosis and treatment design for GBM.
机译:细胞骨架构成细胞控制大小,形状,迁移,增殖变化的主要基础,并形成细胞对其周围环境作出反应的主要手段。实际上,细胞和组织形态不仅常规用于肿瘤分级,而且还用于各种高内涵筛选方法中,目的是鉴定具有治疗潜力的新小分子。这项研究检查了多种胶质母细胞瘤(GBM)中各种细胞骨架调节剂的表达。 GBM是一种非常具有侵略性的疾病,即使经过化学和放射治疗后,其平均寿命也很低。 GBM的癌细胞因其侵袭性,对化学疗法和放射疗法产生抵抗力以及形成继发部位肿瘤的能力而臭名昭著。这项研究旨在深入了解GBM细胞中的细胞骨架调节剂,并了解包括替莫唑胺在内的各种肿瘤药物对细胞骨架调节剂的作用。我们比较了GBM衍生的肿瘤和正常组织,GBM和神经细胞的CD133阳性和阴性细胞以及GBM干样和分化细胞中各种细胞骨架调节剂的表达。另外,检查了细胞骨架调节剂的表达与临床结果之间的相关性,以鉴定与更长患者生存期相关的基因。随后,使用美国食品药品监督管理局(FDA)批准的肿瘤药物进行小分子筛查,并将其对细胞骨架的作用与替莫唑胺进行比较。这项研究确定了对患者生存和肿瘤发展具有重要影响的各种细胞骨架调节剂。重要的是,这项工作强调了使用细胞骨架调节剂作为生物标志物评估GBM的预后和治疗设计的优势。

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