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首页> 外文期刊>BMC Musculoskeletal Disorders >Influence of dendritic polyglycerol sulfates on knee osteoarthritis: an experimental study in the rat osteoarthritis model
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Influence of dendritic polyglycerol sulfates on knee osteoarthritis: an experimental study in the rat osteoarthritis model

机译:树突状聚甘油硫酸盐对膝骨关节炎的影响:在大鼠骨关节炎模型中的实验研究

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Anti-inflammatory nanoparticular compounds could represent a strategy to diminish osteoarthritis (OA) progression. The present study was undertaken to prove the uptake of nanoparticular dendritic polyglycerol sulfates (dPGS) by rat-derived articular chondrocytes and to answer the question of whether dPGS could modulate knee joint cartilage degradation in a rat OA model and whether complications could arise. dPGS uptake and cytotoxicity was assessed in cultured primary rat-derived articular chondrocytes. Subsequently, OA was induced in the right knee joints of 12 male Wistar rats by medial collateral ligament and meniscus transection. Unoperated left knees remained as controls. Six weeks post surgery six rats were either treated daily (14?days) with 30?mg/kg dPGS (s.c.) or a similar volume of physiological saline. Animals were analyzed clinically for gait alterations. Explanted knee joints were studied histologically using OA scores according to Mankin (1971), Glasson et al., (2010) and the synovitis score according to Krenn et al., (2006). Liver, spleen and kidneys were analyzed for degenerative changes due to dPGS accumulation. dPGS was taken up after 2?hours by the chondrocytes. Whereas no significant clinical signs of OA could be detected, at the histological level, all operated rat knee joints revealed features of OA in the medial compartment. The values produced by both OA score systems were lower in rats treated with dPGS compared with saline-treated animals. Synovitis score did not significantly differ between the groups. The analyzed organs revealed no degenerative changes. dPGS presented overall cyto- and biocompatibility, no accumulation in metabolizing organs and chondroprotective properties in the osteoarthritic knee joint.
机译:抗炎纳米颗粒化合物可能代表减少骨关节炎(OA)进展的策略。本研究旨在证明大鼠关节软骨细胞对纳米颗粒状树突状聚甘油硫酸盐(dPGS)的吸收,并回答了dPGS是否可以调节大鼠OA模型中膝关节软骨的降解以及是否会出现并发症。在培养的原代大鼠来源的关节软骨细胞中评估了dPGS的摄取和细胞毒性。随后,通过内侧副韧带和半月板切除术在12只雄性Wistar大鼠的右膝关节中诱发OA。未手术的左膝保持为对照。手术后六周,六只大鼠每天(14天)用30?mg / kg dPGS(s.c.)或类似体积的生理盐水治疗。临床分析动物的步态改变。使用Mankin(1971),Glasson等人(2010)的OA评分和Krenn等人(2006)的滑膜炎评分进行组织学研究。分析了由于dPGS积累引起的肝,脾和肾的退行性变化。 dPGS在2小时后被软骨细胞吸收。尽管没有发现明显的OA临床症状,但在组织学水平上,所有手术的大鼠膝关节均显示了内侧隔室的OA特征。与盐水处理的动物相比,用dPGS处理的大鼠的两种OA评分系统产生的值均较低。滑膜炎评分在两组之间无显着差异。经分析的器官未显示退行性变化。 dPGS表现出总体的细胞和生物相容性,在骨关节炎的膝关节中没有代谢器官的积累和软骨保护特性。

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