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Dual-drug delivery of curcumin and platinum drugs in polymeric micelles enhances the synergistic effects: a double act for the treatment of multidrug-resistant cancer

机译:聚合物胶束中姜黄素和铂类药物的双重给药增强了协同作用:治疗多重耐药性癌症的双重作用

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Combinational chemotherapy is often used to prevent drug induced resistance in cancer. The aim of this work is to test whether the co-delivery of drugs within one nanoparticle can result in increased synergistic effects of both drugs. Therefore, a micelle system with two different compartments, one for the drug curcumin and one for the conjugation of platinum drugs was designed. A triblock copolymer, based on the biodegradable polycaprolactone PCL, a PEG based shell and an amine bearing polymer as the interphase for the conjugation of platinum drugs was prepared by combination of ring-opening polymerization and RAFT polymerization. Curcumin was incorporated into the self-assembled onion-type micelle by physical encapsulation into the PCL core with an entrapment capacity of 6 wt%. The platinum(IV) drug oxoplatin was reacted with succinic anhydride to yield Pt(NH3)(2)Cl-2[(COOH)(2)], which acted as the drug and as a crosslinker for the stabilisation of micelles. The size of the dual drug micelles was measured to be 38 nm by DLS, which was confirmed by TEM. The toxicity of the dual drug delivery system was tested against the A2780 human ovarian cancer cell line and compared with the IC50 value of micelles that deliver either curcumin or the platinum drug alone. The results were analysed using the CalcuSyn software. While curcumin and the platinum drug together without a carrier already showed synergy with a combination index ranging from 0.4 to 0.8, the combined delivery in one nanoparticle did enhance the synergistic effects resulting in a combination index of approximately 0.2-0.35. For comparison, a mixture of two nanoparticles, one with curcumin and the other with the platinum drug, was tested revealing a less noticeable synergistic effect compared to the co-delivery of both drugs in one drug carrier.
机译:联合化疗通常用于预防药物引起的癌症耐药性。这项工作的目的是测试一种纳米颗粒内药物的共同递送是否会导致两种药物的协同作用增强。因此,设计了具有两个不同部分的胶束系统,一个用于姜黄素药物,另一个用于铂药物结合。通过将开环聚合和RAFT聚合相结合,制备了基于可生物降解的聚己内酯PCL,PEG基壳和含胺聚合物作为共轭铂药物中间相的三嵌段共聚物。姜黄素通过物理包封到PCL核中,并以6 wt%的包封能力掺入自组装洋葱型胶束中。使铂(IV)药物氧铂与琥珀酸酐反应,生成Pt(NH3)(2)Cl-2 [(COOH)(2)],其可作为药物和稳定胶束的交联剂。通过DLS测量的双重药物胶束的尺寸为38nm,这通过TEM证实。测试了双重药物递送系统对A2780人卵巢癌细胞系的毒性,并将其与单独递送姜黄素或铂药物的胶束的IC50值进行了比较。使用CalcuSyn软件分析结果。尽管姜黄素和铂药物一起没有载体已经显示出协同作用,其结合指数为0.4到0.8,但是在一个纳米颗粒中的联合递送确实增强了协同作用,导致结合指数约为0.2-0.35。为了进行比较,测试了两种纳米颗粒的混合物,一种与姜黄素,另一种与铂药物混合,与两种药物在一种药物载体中的共同给药相比,其协同作用不太明显。

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