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Dexamethasone-containing biodegradable superparamagnetic microparticles for intra-articular administration: physicochemical and magnetic properties, in vitro and in vivo drug release

机译:用于关节内给药的含地塞米松的可生物降解的超顺磁性微粒:物理化学和磁性,体外和体内药物释放

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摘要

Compared with traditional drug solutions or suspensions, polymeric microparticles represent a valuable means to achieve controlled and prolonged drug delivery into joints, but still suffer from the drawback of limited retention duration in the articular cavity. In this study, our aim was to prepare and characterize magnetic biodegradable microparticles containing dexamethasone acetate (DXM) for intra-articular administration. The superparamagnetic properties, which result from the encapsulation of superparamagnetic iron oxide nanoparticles (SPIONs), allow for microparticle retention with an external magnetic field, thus possibly reducing their clearance from the joint. Two molecular weights of poly(lactic-co-glycolic acid) (PLGA) were used, 12 and 19 kDa. The prepared batches were similar in size (around 10 microm), inner morphology, surface morphology, charge (neutral) and superparamagnetic behaviour. The SPION distribution in the microparticles assessed by TEM indicates a homogeneous distribution and the absence of aggregation, an important factor for preserving superparamagnetic properties. DXM release profiles were shown to be quite similar in vitro (ca. 6 days) and in vivo, using a mouse dorsal air pouch model (ca. 5 days).
机译:与传统的药物溶液或混悬剂相比,聚合物微粒代表了一种实现受控和延长药物向关节内递送的有价值的手段,但仍然存在关节腔内保留时间有限的缺点。在这项研究中,我们的目的是制备和表征包含醋酸地塞米松(DXM)的可生物降解的磁性微粒,用于关节内给药。由超顺磁性氧化铁纳米粒子(SPIONs)的封装产生的超顺磁性质允许微粒在外部磁场的作用下保持,从而可能减少其与关节之间的间隙。使用了两种分子量的聚乳酸-乙醇酸共聚物(PLGA),分别为12和19 kDa。所制备的批次在尺寸(约10微米),内部形态,表面形态,电荷(中性)和超顺磁性行为方面相似。通过TEM评估的微粒中的SPION分布表明分布均匀且不存在聚集,这是保持超顺磁性的重要因素。使用小鼠背气袋模型(约5天),DXM释放曲线在体外(约6天)和体内非常相似。

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