Department of Clinical Sciences, Faculty of Veterinary Medicine, Utrecht University, Utrecht, the Netherlands.
Department of Orthopedics, University Medical Centre Utrecht, Utrecht, the Netherlands.
Osteoarthritis Cartilage. 2023 Mar;31(3):351-362. doi: 10.1016/j.joca.2022.11.008. Epub 2022 Dec 5.
Drug delivery platforms that allow for gradual drug release after intra-articular administration have become of much interest as a treatment strategy for osteoarthritis (OA). The aim of this study was to investigate the safety and efficacy of an intra-articular sustained release formulation containing celecoxib (CXB), a cyclooxygenase-2 (COX-2) selective inhibitor.
Amino acid-based polyesteramide microspheres (PEAMs), a biodegradable and non-toxic platform, were loaded with CXB and employed in two in vivo models of arthritis: an acute inflammatory arthritis model in rats (n = 12), and a randomized controlled study in chronic OA dog patients (n = 30). In parallel, the bioactivity of sustained release of CXB was evaluated in monolayer cultures of primary dog chondrocytes under inflammatory conditions.
Sustained release of CXB did not alleviate acute arthritis signs in the rat arthritis model, based on pain measurements and synovitis severity. However, in OA dog patients, sustained release of CXB improved limb function as objective parameter of pain and quality of life based on gait analysis and owner questionnaires. It also decreased pain medication dependency over a 2-month period and caused no adverse effects. Prostaglandin E levels, a marker for inflammation, were lower in the synovial fluid of CXB-treated dog OA patients and in CXB-treated cultured dog chondrocytes.
These results show that local sustained release of CXB is less suitable to treat acute inflammation in arthritic joints, while safe and effective in treating pain in chronic OA in dogs.
关节内给药后能够实现药物逐渐释放的药物递送平台已成为骨关节炎(OA)治疗策略的研究热点。本研究旨在研究载有塞来昔布(CXB)的关节内缓释制剂的安全性和疗效,CXB 是一种环氧化酶-2(COX-2)选择性抑制剂。
采用氨基酸基聚酯酰胺微球(PEAMs)作为可生物降解且无毒的平台,将 CXB 载入其中,并应用于两种关节炎动物模型:大鼠急性炎症性关节炎模型(n=12)和慢性 OA 犬患者的随机对照研究(n=30)。同时,在炎症条件下单层培养的原代犬软骨细胞中评估 CXB 持续释放的生物活性。
CXB 的持续释放并未减轻大鼠关节炎模型中急性关节炎的体征,根据疼痛测量和滑膜炎严重程度来判断。然而,在 OA 犬患者中,CXB 的持续释放改善了肢体功能,作为疼痛和生活质量的客观参数,基于步态分析和主人问卷。它还降低了 2 个月内的止痛药物依赖性,且无不良反应。CXB 治疗的犬 OA 患者的滑液中以及 CXB 处理的培养犬软骨细胞中的前列腺素 E 水平降低,前列腺素 E 是炎症的标志物。
这些结果表明,局部持续释放 CXB 不太适合治疗关节炎关节的急性炎症,而在治疗犬慢性 OA 的疼痛方面是安全且有效的。
