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首页> 外文期刊>RSC Advances >Magnetically targeted co-delivery of hydrophilic and hydrophobic drugs with hollow mesoporous ferrite nanoparticles
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Magnetically targeted co-delivery of hydrophilic and hydrophobic drugs with hollow mesoporous ferrite nanoparticles

机译:磁性和疏水性药物与空心介孔铁氧体纳米粒子的磁性靶向共同递送

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A magnetically targeted drug delivery system (DDS) is developed to solve the delivery problem of hydrophobic drugs by using hollow mesoporous ferrite nanoparticles (HMFNs). The HMFNs are synthesized by a one-pot hydrothermal method based on the Ostwald ripening process. The biocompatibility of the synthesized HMFNs was determined by MTT assay, lactate dehydrogenase (LDH) leakage assay and hemolyticity against rabbit red blood cells. Moreover, Prussian blue staining and bio-TEM observations showed that the cell uptake of nanocarriers was in a dose and time-dependent manner, and the nanoparticles accumulate mostly in the cytoplasm. A typical highly hydrophobic anti-tuberculosis drug, rifampin (RFP) was loaded into HMFNs using supercritical carbon dioxide (SC-CO _(2) ) impregnation, and the drug loading amount reached as high as 18.25 wt%. In addition, HMFNs could co-encapsulate and co-deliver hydrophobic (RFP) and hydrophilic (isoniazide, INH) drugs simultaneously. The in vitro release tests demonstrated extra sustained co-release profiles of rifampicin and isoniazide from HMFNs. Based on this novel design strategy, the co-delivery of drugs in the same carrier enables a drug delivery system with efficient enhanced chemotherapeutic effect.
机译:开发了一种磁性靶向药物递送系统(DDS),以通过使用中空中孔铁氧体纳米粒子(HMFN)解决疏水性药物的递送问题。 HMFN通过基于奥斯特瓦尔德(Ostwald)成熟过程的一锅水热法合成。通过MTT测定法,乳酸脱氢酶(LDH)泄漏测定法和对兔红细胞的溶血性测定合成的HMFN的生物相容性。此外,普鲁士蓝染色和生物TEM观察表明,纳米载体对细胞的吸收呈剂量和时间依赖性,纳米颗粒主要在细胞质中积累。使用超临界二氧化碳(SC-CO _(2))浸渍法将典型的高疏水性抗结核药物利福平(RFP)加载到HMFN中,药物加载量高达18.25 wt%。另外,HMFNs可以同时共包封和共递送疏水性(RFP)和亲水性(异烟肼,INH)药物。体外释放测试表明,利福平和异烟肼从HMFN释放出额外的持续共释放曲线。基于这种新颖的设计策略,药物在同一载体中的共同递送使得药物递送系统具有有效增强的化学治疗效果。

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