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A Biodegradable Sustained-Released Prednisolone Acetate Microfilm Drug Delivery System Effectively Prolongs Corneal Allograft Survival in the Rat Keratoplasty Model

机译:生物可降解持续释放泼尼松龙醋酸盐微缩膜药物递送系统有效地延长了大鼠角膜移植模型中的角膜同种异体移植存活时间。

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摘要

Frequent and long-term use of topical corticosteroids after corneal transplantation is necessary to prevent graft rejection. However, it relies heavily on patient compliance, and sustained therapeutic drug levels are often not achieved with administration of topical eye drops. A biodegradable drug delivery system with a controlled and sustained drug release may circumvent these limitations. In this study, we investigated the efficacy of a prednisolone acetate (PA)-loaded poly (d,l-lactide-co-ε-caprolactone) (PLC) microfilm drug delivery system on promoting the survival of allogeneic grafts after penetrating keratoplasty (PK) using a rat model. The drug release profiles of the microfilms were characterized (group 1). Subsequently, forty-eight PK were performed in four experimental groups: syngeneic control grafts (group 2), allogeneic control grafts (group 3), allogeneic grafts with subconjunctivally-implanted PA microfilm (group 4), and allogeneic grafts with PA eye drops (group 5; n = 12 in each). PA-loaded microfilm achieved a sustained and steady release at a rate of 0.006–0.009 mg/day, with a consistent aqueous drug concentration of 207–209 ng/ml. The mean survival days was >28 days in group 2, 9.9±0.8 days in group 3, 26.8±2.7 days in group 4, and 26.4±3.4 days in group 5 (P = 0.023 and P = 0.027 compared with group 3). Statistically significant decrease in CD4+, CD163+, CD 25+, and CD54+ cell infiltration was observed in group 4 and group 5 compared with group 3 (P<0.001). There was no significant difference in the mean survival and immunohistochemical analysis between group 4 and group 5. These results showed that sustained PA-loaded microfilm effectively prolongs corneal allograft survival. It is as effective as conventional PA eye drops, providing a promising clinically applicable alternative for patients undergoing corneal transplantation.
机译:角膜移植后经常和长期使用局部皮质类固醇激素对防止移植排斥是必要的。然而,它严重依赖于患者的依从性,并且局部滴眼剂的给药常常不能达到持续的治疗药物水平。具有可控的和持续的药物释放的可生物降解的药物递送系统可能会规避这些限制。在这项研究中,我们调查了醋酸泼尼松龙(PA)负载的聚(d,l-丙交酯-co-ε-己内酯)(PLC)微膜药物递送系统对穿透性角膜移植手术(PK)促进异体移植物存活的功效)使用老鼠模型。表征了微膜的药物释放曲线(第1组)。随后,在四个实验组中进行了四十八次PK:同基因对照移植物(第2组),同种异体对照移植物(第3组),具有结膜下植入的PA微膜的同种异体移植物(第4组)和具有PA滴眼液的同种异体移植物(第4组)第5组; n = 12)。装有PA的缩微胶片以0.006-0.009 mg /天的速率实现了持续稳定的释放,药物水溶液的稳定浓度为207-209 ng / ml。第2组平均生存天数> 28天,第3组为9.9±0.8天,第4组为26.8±2.7天,第5组为26.4±3.4天(与第3组相比,P = 0.023和P = 0.027)。与第3组相比,在第4组和第5组中观察到CD4 +,CD163 +,CD 25+和CD54 +细胞浸润的统计学显着降低(P <0.001)。第4组和第5组之间的平均存活率和免疫组化分析无显着差异。这些结果表明,持续加载PA的微膜可以有效延长同种异体角膜的存活。它与常规PA滴眼液一样有效,为进行角膜移植的患者提供了有希望的临床应用替代方案。

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