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首页> 外文期刊>Cancer research: The official organ of the American Association for Cancer Research, Inc >Intratumoral therapy of glioblastoma multiforme using genetically engineered transferrin for drug delivery.
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Intratumoral therapy of glioblastoma multiforme using genetically engineered transferrin for drug delivery.

机译:使用基因工程转铁蛋白进行药物递送的多形性胶质母细胞瘤的肿瘤内治疗。

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Glioblastoma multiforme (GBM) is the most common and lethal primary brain tumor with median survival of only 12 to 15 months under the current standard of care. To both increase tumor specificity and decrease nonspecific side effects, recent experimental strategies in the treatment of GBM have focused on targeting cell surface receptors, including the transferrin (Tf) receptor, that are overexpressed in many cancers. A major limitation of Tf-based therapeutics is the short association of Tf within the cell to deliver its payload. We previously developed two mutant Tf molecules, K206E/R632A Tf and K206E/K534A Tf, in which iron is locked into each of the two homologous lobes. Relative to wild-type Tf, we showed enhanced delivery of diphtheria toxin (DT) from these mutants to a monolayer culture of HeLa cells. Here, we extend the application of our Tf mutants to the treatment of GBM. In vitro treatment of Tf mutants to a monolayer culture of glioma cells showed enhanced cellular association as well as enhanced delivery of conjugated DT. Treatment of GBM xenografts with mutant Tf-conjugated DT resulted in pronounced regression in vivo, indicating their potential use as drug carriers.
机译:多形性胶质母细胞瘤(GBM)是最常见的致死性原发性脑肿瘤,在目前的护理标准下,中位生存期仅为12至15个月。为了既增加肿瘤特异性又减少非特异性副作用,最近治疗GBM的实验策略集中在靶向在许多癌症中过表达的细胞表面受体,包括转铁蛋白(Tf)受体。基于Tf的治疗方法的主要局限性是Tf在细胞内传递其有效载荷的时间短。我们先前开发了两个突变Tf分子,即K206E / R632A Tf和K206E / K534A Tf,其中铁被锁定在两个同源叶的每一个中。相对于野生型Tf,我们显示出从这些突变体到HeLa细胞单层培养的白喉毒素(DT)传递增强。在这里,我们将Tf突变体的应用扩展到GBM的治疗。 Tf突变体对神经胶质瘤细胞单层培养的体外治疗显示增强的细胞结合以及结合DT的传递。用突变的Tf-缀合的DT处理GBM异种移植物导致体内明显消退,表明它们潜在地用作药物载体。

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