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A novel dexamethasone-loaded liposome alleviates rheumatoid arthritis in rats

机译:一种新的地塞米松加载的脂质体减轻了大鼠类风湿性关节炎

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摘要

In this study, an inflammation-targeted delivery system based on a liposomal carrier was developed to deliver hydrophobic dexamethasone against arthritis. Using two FDA-approved excipients for intravenous injection, dexamethasone loaded liposome (Dex-Lip) was prepared by a thin-film hydration method. The biodistribution of 1,1'-dioctadecyl-3,3,3',3'-tetramethylindodicarbocyanine-loaded liposomes (DiD-Lips) were performed in rats with adjuvant-induced arthritis and demonstrated specific targeting efficacy in the disease site. DiD-Lips showed prolonged retention time in the inflammatory joint tissues compared with free DiD. Dex-Lips effectively suppressed the joint swelling in arthritis rats and significantly down-regulated serum pro-inflammatory cytokines including tumor necrosis factor-alpha and interleukin-1 beta when compared to free dexamethasone. Furthermore, Dex-Lips had no significantly impact on the body weight, alleviated the hyperglycemia and improved haematological profiles of rheumatoid arthritis rats during the treatment process. Taken together, a safe liposomal delivery system was developed to achieve inflammation targeted therapy against arthritis.
机译:在该研究中,开发了基于脂质体载体的炎症靶向递送系统,以促进疏水性地塞米松免受关节炎。使用两种FDA批准的静脉注射辅助剂,通过薄膜水合方法制备地塞米松装载脂质体(DEX-唇)。在具有佐剂诱导的关节炎的大鼠中,在大鼠中进行1,1'-二烯至癸酰-3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3,3'。与自由相比,DID-LIPS在炎症关节组织中显示出长时间的保留时间。 Dex-Lips有效地抑制了关节炎大鼠的关节肿胀,并且显着下调血清促炎细胞因子,包括与游离地塞米松相比的肿瘤坏死因子-α和白细胞介素-1β。此外,Dex-Lips对体重没有显着影响,缓解高血糖和改善了类风湿性关节炎大鼠的治疗过程中的血清湿性血液谱。一起服用,开发了一种安全的脂质体递送系统,以实现针对关节炎的炎症靶向治疗。

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