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Biodegradable Polymersomes for the Delivery of Gemcitabine to Panc-1 Cells

机译:吉西他滨向Panc-1细胞传递的可生物降解聚合物

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Traditional anticancer chemotherapy often displays toxic side effects, poor bioavailability, and a low therapeutic index. Targeting and controlled release of a chemotherapeutic agent can increase drug bioavailability, mitigate undesirable side effects, and increase the therapeutic index. Here we report a polymersome-based system to deliver gemcitabine to Panc-1 cellsin vitro. The polymersomes were self-assembled from a biocompatible and completely biodegradable polymer, poly(ethylene oxide)-poly(caprolactone), PEO-PCL. We showed that we can encapsulate gemcitabine within stable 200 nm vesicles with a 10% loading efficiency. These vesicles displayed a controlled release of gemcitabine with 60% release after 2 days at physiological pH. Upon treatment of Panc-1 cellsin vitro, vesicles were internalized as verified with fluorescently labeled polymersomes. Clonogenic assays to determine cell survival were performed by treating Panc-1 cells with varying concentrations of unencapsulated gemcitabine (FreeGem) and polymersome-encapsulated gemcitabine (PolyGem) for 48 hours. 1 μM PolyGem was equivalent in tumor cell toxicity to 1 μM FreeGem, with a one log cell kill observed. These studies suggest that further investigation on polymersome-based drug formulations is warranted for chemotherapy of pancreatic cancer.
机译:传统的抗癌化学疗法通常会显示毒性副作用,不良的生物利用度和较低的治疗指数。靶向和控制释放化疗药物可以提高药物的生物利用度,减轻不良副作用,并提高治疗指数。在这里,我们报告了一个基于聚合物的系统,可将吉西他滨在体外递送给Panc-1细胞。聚合物囊泡是由生物相容性和完全可生物降解的聚合物,聚(环氧乙烷)-聚(己内酯),PEO-PCL自组装而成。我们表明,我们可以将吉西他滨包封在稳定的200nm囊泡中,负载效率为10%。这些囊泡在生理pH下2天后显示出吉西他滨的控释和60%释放。在体外处理Panc-1细胞后,囊泡被内化,如荧光标记的聚合物囊泡所证实。通过用不同浓度的未包封的吉西他滨(FreeGem)和聚合物囊体包埋的吉西他滨(PolyGem)处理Panc-1细胞进行克隆试验,以确定细胞存活时间,持续48小时。 1μMPolyGem在肿瘤细胞毒性方面与1μMFreeGem相当,观察到对数细胞杀死。这些研究表明,对基于多聚体的药物制剂进行胰腺癌化疗的进一步研究是必要的。

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