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Lentiviral Vectors as Tools for the Study and Treatment of Glioblastoma

机译:慢病毒载体作为胶质母细胞瘤研究和治疗的工具

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Glioblastoma (GBM) has the worst prognosis among brain tumors, hence basic biology, preclinical, and clinical studies are necessary to design effective strategies to defeat this disease. Gene transfer vectors derived from the most-studied lentivirus—the Human Immunodeficiency Virus type 1—have wide application in dissecting GBM specific features to identify potential therapeutic targets. Last-generation lentiviruses (LV), highly improved in safety profile and gene transfer capacity, are also largely employed as delivery systems of therapeutic molecules to be employed in gene therapy (GT) approaches. LV were initially used in GT protocols aimed at the expression of suicide factors to induce GBM cell death. Subsequently, LV were adopted to either express small noncoding RNAs to affect different aspects of GBM biology or to overcome the resistance to both chemo- and radiotherapy that easily develop in this tumor after initial therapy. Newer frontiers include adoption of LV for engineering T cells to express chimeric antigen receptors recognizing specific GBM antigens, or for transducing specific cell types that, due to their biological properties, can function as carriers of therapeutic molecules to the cancer mass. Finally, LV allow the setting up of improved animal models crucial for the validation of GBM specific therapies.
机译:胶质母细胞瘤(GBM)在脑肿瘤中的预后最差,因此需要基本的生物学,临床前和临床研究来设计有效的策略来战胜这种疾病。源自研究最多的慢病毒(人类免疫缺陷病毒1型)的基因转移载体在剖析GBM特定特征以鉴定潜在治疗靶点方面具有广泛的应用。安全性和基因转移能力大大提高的上一代慢病毒(LV)也被大量用作基因治疗(GT)方法中使用的治疗性分子的递送系统。 LV最初用于GT方案,旨在表达自杀因子以诱导GBM细胞死亡。随后,LV被用于表达小的非编码RNA来影响GBM生物学的不同方面,或者克服了在初始治疗后容易在该肿瘤中发生的化学疗法和放射疗法的耐药性。较新的领域包括采用LV技术改造T细胞,以表达识别特定GBM抗原的嵌合抗原受体,或转导由于其生物学特性而可以充当癌症分子治疗分子载体的特定细胞类型。最后,LV允许建立对验证GBM特定疗法至关重要的改良动物模型。

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