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首页> 外文期刊>Pharmaceutical research >In Vitro ’, ‘ In Vivo ’ and ‘ In Silico ’ Investigation of the Anticancer Effectiveness of Oxygen-Loaded Chitosan-Shelled Nanodroplets as Potential Drug Vector
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In Vitro ’, ‘ In Vivo ’ and ‘ In Silico ’ Investigation of the Anticancer Effectiveness of Oxygen-Loaded Chitosan-Shelled Nanodroplets as Potential Drug Vector

机译:体外','体内'和'在硅的抗癌耐壳壳聚糖壳纳米电池抗癌效能调查中作为潜在的药物载体

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ABSTRACT Purpose Chitosan-shelled/decafluoropentane-cored oxygen-loaded nanodroplets (OLN) are a new class of nanodevices to effectively deliver anti-cancer drugs to tumoral cells. This study investigated their antitumoral effects per se , using a mathematical model validated on experimental data . Methods OLN were prepared and characterized either in vitro or in vivo. TUBO cells, established from a lobular carcinoma of a BALB-neuT mouse, were investigated following 48爃 of incubation in the absence/presence of different concentrations of OLN. OLN internalization, cell viability, necrosis, apoptosis, cell cycle and reactive oxygen species (ROS) production were checked as described in the Method section. In vivo tumor growth was evaluated after subcutaneous transplant in BALB/c mice of TUBO cells either without treatment or after 24爃 incubation with 10% v / v OLN. Results OLN showed sizes of about 350爊m and a positive surface charge (45爉V). Dose-dependent TUBO cell death through ROS-triggered apoptosis following OLN internalization was detected. A mathematical model predicting the effects of OLN uptake was validated on both in vitro and in vivo results. Conclusions Due to their intrinsic toxicity OLN might be considered an adjuvant tool suitable to deliver their therapeutic cargo intracellularly and may be proposed as promising combined delivery system.
机译:摘要目的壳聚糖 - 壳/甲基氟戊烷 - 芯载氧纳米油(OLN)是一类新的纳米纳米型纳米型,有效地将抗癌药物递给肿瘤细胞。本研究通过在实验数据上验证的数学模型研究了它们的抗肿瘤效应本身。方法在体外或体内制备oln并表征。在不存在/存在不同浓度OLN的情况下,在48‰的孵育后研究了从BALB-光学鼠的小甲状腺癌建立的诱导细胞。如方法部分所述,检查OLN内化,细胞活力,坏死,细胞凋亡,细胞周期和反应性氧物质(ROS)产生。在没有治疗的BALB / C小小鼠的皮下移植的情况下在皮下移植后或用10%v / v OLN孵育后,在皮下移植后进行体内肿瘤生长。结果OLN显示约350米米和正面电荷(45℉)的尺寸。检测到OLN内化后通过ROS触发凋亡的剂量依赖性TUBO细胞死亡。在体外和体内验证预测OLN摄取效果的数学模型。由于其内在毒性OLN的结论可能被认为是适合于细胞内递送其治疗性货物的佐剂工具,并且可以提出作为有前途的联合递送系统。

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