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关节内负载洛索洛芬的 PLGA 微球:在治疗骨关节炎方面提高治疗效果和降低全身毒性。

Intra-articular lornoxicam loaded PLGA microspheres: enhanced therapeutic efficiency and decreased systemic toxicity in the treatment of osteoarthritis.

机构信息

Department of Pharmaceutics, School of Pharmaceutical Science, Shandong University, China.

出版信息

Drug Deliv. 2012 Jun-Jul;19(5):255-63. doi: 10.3109/10717544.2012.700962. Epub 2012 Jul 9.

DOI:10.3109/10717544.2012.700962
PMID:22775466
Abstract

The aim of this study was to investigate the joint tissue distribution and pharmacodynamics of Lornoxicam (Lnxc) following intra-articular injection of either Lnxc suspensions or sustained release Lnxc-loaded PLGA microspheres (Lnxc-MS), as well as the biocompatibility of PLGA microspheres with or without drugs. In this study, Lnxc suspensions or Lnxc-loaded PLGA microspheres was injected into the knee joint cavity of rats. Blood samples were taken at predetermined times from the jugular vein and the joint tissue (cartilage and synovial membrane) were removed from the rats. Biocompatibility and pharmacodynamics were evaluated by observing the swelling of the joints of the rats and histological analysis following the injection of the microspheres. The plasma drug concentration decreased in rats and retention time increased in rats' joint with intra-articular injections of microspheres, revealing good targeting efficiency and decreased systemic toxicity. After 30 days of intra-articular injection with Lnxc-loaded or blank microspheres, the filtration liquid accumulation, blood vessels and fibrous proliferation were not detected, showing their good compatibility. Furthermore, the articular cartilage damage by papain could also be repaired by the Lnxc-loaded PLGA microspheres. In conclusion, intra-articular Lnxc-MS have considerable potential for creating a sustained release Lnxc delivery system and providing effective healing to Osteoarthritis.

摘要

本研究旨在探讨洛索洛芬(Lnxc)关节内注射混悬液或载药 PLGA 微球(Lnxc-MS)后在关节组织中的分布和药效学,以及载药和非载药 PLGA 微球的生物相容性。本研究将 Lnxc 混悬液或 Lnxc 载药 PLGA 微球注入大鼠膝关节腔,从颈静脉取血,取大鼠关节软骨和滑膜组织。通过观察微球注射后大鼠关节肿胀和组织学分析,评价其生物相容性和药效学。微球关节内注射后,大鼠血浆药物浓度降低,关节内保留时间延长,显示出良好的靶向效率和降低的全身毒性。在关节内注射载药或空白微球 30 天后,未检测到滤过液积聚、血管和纤维增生,显示出良好的相容性。此外,载药 PLGA 微球还可修复木瓜蛋白酶引起的关节软骨损伤。综上所述,关节内 Lnxc-MS 具有作为一种新型 Lnxc 持续释放给药系统的潜力,可有效治疗骨关节炎。

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