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Amphiphilic hyper-branched co-polymer nanoparticles for the controlled delivery of anti-tumor agents.

机译:两亲性超支化共聚物纳米粒子,用于控制抗肿瘤药物的递送。

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In this investigation, we have designed and synthesized an amphiphilic co-polymer with hyper-branched poly(amine-ester) and polylactide (HPAE-co-PLA) to generate nanoparticles (NPs). These have been used to encapsulate a highly active hydrophobic anti-tumor agent, 2-benzoylpyridine 4-ethyl-3-thiosemicarbazone (Bp4eT). Encapsulation in NPs was done in an effort to increase the anti-tumor activity of this agent by facilitating its delivery to tumor cells. We have also examined and optimized the formulation parameters of the NPs that alter their drug-loading capacity and their physical, chemical and biological properties. The resulting NPs exhibited high Bp4eT-loading capacity and substantial stability in aqueous solution. In vitro drug release studies demonstrated a controlled drug release profile with increased release at acidic pH. Anti-tumor proliferation assays showed that both free drug and drug-encapsulated NPs markedly inhibited tumor cell proliferation in a time- and concentration-dependent manner. Direct microscopic observation revealed that the fluorescent NPs were taken up by cells and localized, in part, in organelles consistent with lysosomes. These results demonstrate a feasible application of the amphiphilic hyper-branched co-polymer, HPAE-co-PLA, as nanocarriers for intracellular delivery of potent anti-tumor agents.
机译:在这项研究中,我们设计并合成了具有超支化聚(胺酯)和聚丙交酯(HPAE-co-PLA)的两亲共聚物,以生成纳米粒子(NP)。这些已被用于封装高活性疏水抗肿瘤剂,2-苯甲酰基吡啶4-乙基-3-硫代半碳酰胺(Bp4eT)。进行NP中的封装是为了通过促进其向肿瘤细胞的递送来增加该试剂的抗肿瘤活性。我们还检查并优化了NP的配方参数,这些参数改变了它们的载药量及其物理,化学和生物学特性。所得NP显示出高的Bp4eT负载能力和在水溶液中的基本稳定性。体外药物释放研究表明,药物的控制释放曲线在酸性pH下具有增加的释放。抗肿瘤增殖试验表明,游离药物和药物包封的NP均以时间和浓度依赖性方式显着抑制肿瘤细胞的增殖。直接显微镜观察显示,荧光NP被细胞吸收并部分定位在与溶酶体一致的细胞器中。这些结果证明了两亲性超支化共聚物HPAE-co-PLA作为纳米载体在细胞内递送有效抗肿瘤剂的可行应用。

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