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Recent advances in intra-articular drug delivery systems to extend drug retention in joint

机译:关节内药物递送系统的最新进展,以延长关节药物保留

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Intra-articular (IA) administration of therapeutic agents has been employed to selectively deliver active compounds at their site of action for the treatment of chronic joint diseases such as osteoarthritis, rheumatoid arthritis, and joint pain. Direct IA delivery of active compounds to local tissues occasionally provides improved therapeutic outcomes with reduced dose, while minimizing systemic exposure and undesirable adverse effects. However, many small drugs (< 10,000 Da) administered intra-articularly, tend to be rapidly effluxed from the synovium into the blood stream, thus requiring frequent IA injection. To date, different pharmaceutical approaches have been investigated, including polymer and/or lipid-based nanoparticles (NPs), microparticles (MPs), conventional and/or thermo-responsive hydrogels, drug suspension, and oily depot systems, to prolong the drug retention time in the joint, thus improving the pharmacokinetic profile and/or the therapeutic efficacy of active compounds. Herein, we have summarized the recent research trends on IA delivery systems with a focus on NPs, MPs, and hydrogel system, which have been studied most extensively to achieve extended retention time following IA injection.
机译:术中(IA)的治疗剂施用治疗剂在其作用部位选择性地递送活性化合物,用于治疗慢性关节疾病,如骨关节炎,类风湿性关节炎和关节疼痛。将活性化合物的直接递送到局部组织偶尔提供改善的治疗结果,减少剂量,同时最小化系统性暴露和不期望的不良影响。然而,关节内施用的许多小药物(<10,000da)往往将从Synovium迅速流出到血流中,因此需要频繁注射Ia注射。迄今为止,已经研究了不同的药物方法,包括聚合物和/或脂质的纳米颗粒(NPS),微粒(MPS),常规和/或热响应水凝胶,药物悬浮液和油性仓库系统,以延长药物保留在关节中的时间,从而改善了药代动力学曲线和/或活性化合物的治疗效果。在此,我们已经总结了最近的IA递送系统的研究趋势,其专注于NPS,MP和水凝胶系统,这些趋势已经过度研究了IA注射液后的延长保留时间。

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