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首页> 外文期刊>Materials science & engineering >Reactive oxygen species-responsive amino acid-based polymeric nanovehicles for tumor-selective anticancer drug delivery
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Reactive oxygen species-responsive amino acid-based polymeric nanovehicles for tumor-selective anticancer drug delivery

机译:活性氧物种响应性氨基酸基聚合物纳米车辆用于肿瘤选择性抗癌药物的递送

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摘要

Stimuli-triggered drug delivery systems have been recognized as a crucial strategy to achieve on-demand drug release at the tumor for improving therapeutic efficacy. In this work, novel biocompatible and biodegradable reactive oxygen species (ROS)-responsive amino acid-based polymeric micelles were developed for tumor-specific drug release triggered by high ROS levels in cancer cells, which were composed of amphiphilic poly (aspartic acid) (PASP) derivatives (PASP-BSer) with phenylborate serine (BSer) side groups as the ROS-responsive unit. A series of PASP-BSer conjugates with different degree of substitution (DS) were synthesized, and their self-assembly and H2O2-responsive behaviors were investigated to optimize the structure of PASP-BSer. In vitro drug loading and release studies confirmed that the optimized PASP-BSer micelles could effectively encapsulate the model anticancer drug doxorubicin (Dox) and exhibit desirable H2O2-triggered release behaviors. More importantly, Dox-loaded PASP-BSer micelles showed high selective cytotoxicity against A549 cancer cells than L929 normal cells. Accordingly, PASP-BSer micelles have significant potential as on-demand drug carriers for anticancer therapy.
机译:刺激触发的药物输送系统已被认为是实现按需释放药物以改善治疗效果的关键策略。在这项工作中,针对由癌细胞中高ROS水平触发的肿瘤特异性药物释放,开发了基于生物相容性和可生物降解的活性氧(ROS)响应型氨基酸的高分子胶束,该药物由两亲性聚天冬氨酸组成(具有苯硼酸丝氨酸(BSer)侧基作为ROS响应单元的PASP)衍生物(PASP-BSer)。合成了一系列具有不同取代度(DS)的PASP-BSer缀合物,并研究了它们的自组装和H2O2响应行为,以优化PASP-BSer的结构。体外药物加载和释放研究证实,优化的PASP-BSer胶束可以有效地封装模型抗癌药物阿霉素(Dox),并表现出理想的H2O2触发的释放行为。更重要的是,与L929正常细胞相比,载有Dox的PASP-BSer胶束对A549癌细胞具有较高的选择性细胞毒性。因此,PASP-BSer胶束作为抗癌治疗的按需药物载体具有巨大潜力。

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