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Injectable nanoparticle-loaded hydrogel system for local delivery of sodium alendronate

机译:注射用纳米颗粒负载水凝胶系统,用于局部递送阿仑膦酸钠

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摘要

Systemic administration of bisphosphonates, e.g. sodium alendronate (Aln) is characterized by extremely low bioavailability and high toxicity. To omit aforementioned drawbacks an injectable system for the intra-bone delivery of Aln based on Aln-loaded nanoparticles (NPs-Aln) suspended in a hydrogel matrix (gellan gum, GG) was developed. Aln was encapsulated in poly(lactide-co-glycolide) (PLGA 85:15) by solid-oil-water emulsification. Drug release tests showed that within 25 days all the encapsulated drug was released from NPs-Aln and the release rate was highest at the beginning and decreased with time. In contrast, by suspending NPs-Aln in a GG matrix, the release rate was significantly lower and more constant in time. The GG-NPs-Aln system was engineered to be easily injectable and was able to reassemble its structure after extrusion as shown by rheological measurements. In vitro studies showed that the GG-NPs-Aln was cytocompatible with MG-63 osteoblast-like cells and it inhibited RANKL-mediated osteoclastic differentiation of RAW 264.7 cells. The injectability, the sustained local delivery of small doses of Aln and the biological activity render the GG-NPs-Aln system promising for the local treatment of osteoporosis and other bone tissue disorders. (C) 2015 Elsevier B.V. All rights reserved.
机译:双膦酸盐的全身给药,例如阿仑膦酸钠(Aln)的特征在于极低的生物利用度和高毒性。为了消除上述缺点,开发了基于悬浮在水凝胶基质(结冷胶,GG)中的载有Aln的纳米颗粒(NPs-Aln)用于Aln骨内递送的注射系统。通过固体油水乳化将Aln封装在聚(丙交酯-共-乙交酯)(PLGA 85:15)中。药物释放测试表明,在25天内,所有封装的药物都从NPs-Aln中释放出来,释放速率在开始时最高,并随时间降低。相反,通过将NPs-Aln悬浮在GG基质中,释放速率显着降低,并且在时间上更加恒定。 GG-NPs-Aln系统经过精心设计,易于注射,在挤出后能够重组其结构,如流变学测量所示。体外研究表明,GG-NPs-Aln与MG-63成骨细胞样细胞具有细胞相容性,并抑制RANKL介导的R​​AW 264.7细胞的破骨细胞分化。可注射性,小剂量Aln的持续局部递送和生物活性使GG-NPs-Aln系统有望用于骨质疏松症和其他骨组织疾病的局部治疗。 (C)2015 Elsevier B.V.保留所有权利。

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