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可降解聚(乙二醇)水凝胶微球作为载体制备缓控释药物:关节内命运。

Intra-articular fate of degradable poly(ethyleneglycol)-hydrogel microspheres as carriers for sustained drug delivery.

机构信息

Occlugel, Archimed, 12 rue Charles de Gaulle, 78350 Jouy en Josas, France.

出版信息

Int J Pharm. 2013 Nov 18;456(2):536-44. doi: 10.1016/j.ijpharm.2013.08.016. Epub 2013 Aug 24.

DOI:10.1016/j.ijpharm.2013.08.016
PMID:23978631
Abstract

A novel degradable microsphere (MS) for intra-articular drug delivery, composed of a polyethylene glycol (PEG) core containing degradable regions made of short poly-(lactic-co-glycolic acid) (PLGA) sequences - named PEG-hydrogel MS - was injected into the cavity of sheep shoulder joint, and compared to non-degradable MS devoid of hydrolysable crosslinker in terms of location, degradation and inflammation. One week after intra-articular injection both groups of MS were localized beneath the synovial lining of the synovial fringes located at bottom of the shoulder joint, while a fraction of particles remained in synovial fluid. Histological analyses made one and 4 weeks after intra-articular injection showed cell proliferation around the non-degradable MS entrapped within the synovium. By contrast, degradable PEG-hydrogel MS were surrounded by few cells. The degradation of degradable PEG-hydrogel MS within the synovium was slow and was not fully complete after four weeks. Our findings indicate that the tissue entrapment of MS below the synovial lining was independent of the material degradability, while degradable PEG-hydrogel MS are less inflammatory than the non-degradable one. Degradable PEG-hydrogel MS offer several advantages over the non-degradable MS as carriers for a sustained drug delivery in synovial tissue according to the low intensity of inflammatory reaction triggered in synovium.

摘要

一种新型可降解微球(MS)用于关节内药物输送,由包含可降解区域的聚乙二醇(PEG)核心组成,该区域由短聚(乳酸-共-乙醇酸)(PLGA)序列制成 - 命名为 PEG-水凝胶 MS - 被注入到羊肩关节的腔中,并与不含可水解交联剂的不可降解 MS 进行比较,比较它们的位置、降解和炎症情况。在关节内注射后一周,两组 MS 都定位于位于肩关节底部的滑膜边缘的滑膜衬里下方,而一部分颗粒仍存在于滑液中。关节内注射后 1 周和 4 周进行的组织学分析显示,不可降解 MS 被包裹在滑膜内周围有细胞增殖。相比之下,可降解的 PEG-水凝胶 MS 周围只有少量细胞。在滑膜内,可降解的 PEG-水凝胶 MS 的降解速度较慢,四周后仍未完全降解。我们的研究结果表明,MS 在滑膜衬里下方的组织内捕获与材料的可降解性无关,而可降解的 PEG-水凝胶 MS 比不可降解的 MS 炎症反应程度更低。与不可降解 MS 相比,可降解的 PEG-水凝胶 MS 作为在滑膜组织中进行持续药物输送的载体具有几个优势,因为它在滑膜中引发的炎症反应强度较低。

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