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丝纳米粒子的 pH 依赖性抗癌药物释放。

pH-dependent anticancer drug release from silk nanoparticles.

机构信息

Tufts University, Department of Biomedical Engineering, 4 Colby Street, Medford, MA 02155, USA.

出版信息

Adv Healthc Mater. 2013 Dec;2(12):1606-11. doi: 10.1002/adhm.201300034. Epub 2013 Apr 26.

Abstract

Silk has traditionally been used as a suture material because of its excellent mechanical properties and biocompatibility. These properties have led to the development of different silk-based material formats for tissue engineering and regenerative medicine. Although there have been a small number of studies about the use of silk particles for drug delivery, none of these studies have assessed the potential of silk to act as a stimulus-responsive anticancer nanomedicine. This report demonstrates that an acetone precipitation of silk allows the formation of uniform silk nanoparticles (98 nm diameter, polydispersity index 0.109), with an overall negative surface charge (-33.6 ± 5.8 mV), in a single step. Silk nanoparticles are readily loaded with doxorubicin (40 ng doxorubicin/μg silk) and show pH-dependent release (pH 4.5≫ 6.0 > 7.4). In vitro studies with human breast cancer cell lines demonstrates that the silk nanoparticles are not cytotoxic (IC50 > 120 μg mL(-1) ) and that doxorubicin-loaded silk nanoparticles are able to overcome drug resistance mechanisms. Live cell fluorescence microscopy studies show endocytic uptake and lysosomal accumulation of silk nanoparticles. In summary, the pH-dependent drug release and lysosomal accumulation of silk nanoparticles demonstrate the ability of drug-loaded silk nanoparticles to serve as a lysosomotropic anticancer nanomedicine.

摘要

传统上,由于其优异的机械性能和生物相容性,丝被用作缝合材料。这些特性导致了不同的丝基材料格式的发展,用于组织工程和再生医学。尽管已经有少量关于丝颗粒用于药物传递的研究,但这些研究都没有评估丝作为刺激响应性抗癌纳米药物的潜力。本报告表明,丝的丙酮沉淀允许在单个步骤中形成均匀的丝纳米颗粒(98nm 直径,多分散指数 0.109),具有整体负表面电荷(-33.6±5.8mV)。丝纳米颗粒易于负载阿霉素(40ng 阿霉素/μg 丝),并表现出 pH 依赖性释放(pH4.5≫6.0>7.4)。体外研究人类乳腺癌细胞系表明,丝纳米颗粒没有细胞毒性(IC50>120μgmL(-1)),并且负载阿霉素的丝纳米颗粒能够克服耐药机制。活细胞荧光显微镜研究表明丝纳米颗粒的内吞作用和溶酶体积累。总之,丝纳米颗粒的 pH 依赖性药物释放和溶酶体积累证明了负载药物的丝纳米颗粒作为溶酶体型抗癌纳米药物的能力。

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