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首页> 外文期刊>International Journal of Pharmaceutics >Sugar-modified poly(propylene imine) dendrimers as drug delivery agents for cytarabine to overcome drug resistance
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Sugar-modified poly(propylene imine) dendrimers as drug delivery agents for cytarabine to overcome drug resistance

机译:糖改性聚(丙烯亚胺)树枝状大分子作为用于克服耐药性的油炸药递送剂

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摘要

Maltose-modified poly(propylene imine) glycodendrimers (PPI-m OS) of the 4th generation provide a promising strategy for leukemia treatment. Anticancer therapy with nucleoside analog drugs such as cytarabine (Ara-C) frequently has limited efficacy due to drug resistance, inefficient uptake and accumulation of the drug inside cancer cells where it has to be transformed into the active triphosphate congener. The cationic nature of PPI dendrimers makes it possible to form complexes with nucleotide Ara-C triphosphate forms (Ara-CTP). The aim of this work was to test the concept of applying PPI glycodendrimers as drug delivery devices in order to facilitate the delivery of activated cytarabine to cancer cells to overcome metabolic limitations of the drug. The study has been carried out using 1301 and HL-60 leukemic cell lines as well as peripheral blood mononuclear cells. The results of cytotoxicity and apoptosis assays showed enhanced activity of Ara-C triphosphate form (Ara-CTP) complexed with PPI-m dendrimers in relation to free Ara-C and Ara-CTP against 1301 leukemic cells. Secondly, enhanced uptake and cytotoxicity of Ara-CTP-dendrimers complexes toward 1301 cells with blocked human equilibrative nucleoside transporter - hENT1 suggested that this combination might be a versatile candidate for chemotherapy against resistant acute lymphoblastic leukemia cells with lower expression of hENT1. (C) 2016 Elsevier B.V. All rights reserved.
机译:第4代的麦芽糖 - 改性的聚(丙烯亚胺)glycodendrimers(PPI-M OS)提供一种用于治疗白血病的有希望的策略。与核苷类似物药物如阿糖胞苷(阿糖胞苷)抗癌疗法常常具有有限的功效由于耐药性,低效率的摄取和癌症细胞内的药物,其中它必须被转化为活性三磷酸同类的积累。 PPI树枝状聚合物的阳离子性质使得有可能形成具有核苷酸阿糖胞苷三磷酸形式(ARA-CTP)的复合物。这项工作的目的是测试,以便于对癌细胞递送活化的阿糖胞苷,以克服药物代谢限制施加PPI glycodendrimers作为药物递送装置的概念。该研究已进行了使用1301和HL-60白血病细胞系以及外周血单核细胞。细胞毒性和凋亡测定法的结果表现出增强的关于与PPI-m的树枝状聚合物络合游离阿糖胞苷阿糖胞苷和-CTP针对1301个白血病细胞阿糖胞苷三磷酸酯形式(ARA-CTP)的活性。其次,增强阿糖胞苷CTP-树枝状聚合物复合物的摄取和细胞毒性朝向1301个细胞与人类阻断平衡型核苷转运 - hENT1建议该组合可以是一个通用的候选对耐急性淋巴细胞白血病细胞化疗hENT1的较低表达。 (c)2016 Elsevier B.v.保留所有权利。

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