透明质酸
自愈水凝胶
生物相容性
莱菔硫烷
化学
骨关节炎
药物输送
药理学
生物化学
医学
解剖
病理
有机化学
替代医学
作者
Mônica Helena Monteiro do Nascimento,Felipe Nogueira Ambrosio,Débora Carajiliascov Ferraraz,Hermann Windisch-Neto,Samyr Machado Querobino,Michelle Nascimento-Sales,Carlos Alberto-Silva,Marcelo A. Christoffolete,Margareth K.K.D. Franco,Ben Kent,Fabiano Yokaichiya,Christiane Bertachini Lombello,Daniele Ribeiro de Araújo
标识
DOI:10.1016/j.msec.2021.112345
摘要
Sulforaphane (SFN) is an isothiocyanate with anti-arthritic and immuno-regulatory activities, supported by the downregulation of NF-κB pathway, reduction on metalloproteinases expression and prevention of cytokine-induced cartilage degeneration implicated in OA progression. SFN promising pharmacological effects associated to its possible use, by intra-articular route and directly in contact to the site of action, highlight SFN as promising candidate for the development of drug-delivery systems. The association of poloxamers (PL) and hyaluronic acid (HA) supports the development of osteotrophic and chondroprotective pharmaceutical formulations. This study aims to develop PL-HA hybrid hydrogels as delivery systems for SFN intra-articular release and evaluate their biocompatibility and efficacy for osteoarthritis treatment. All formulations showed viscoelastic behavior and cubic phase organization. SFN incorporation and drug loading showed a concentration-dependent behavior following HA addition. Drug release profiles were influenced by both diffusion and relaxation of polymeric chains mechanisms. The PL407-PL338-HA-SFN hydrogel did not evoke pronounced cytotoxic effects on either osteoblast or chondrosarcoma cell lines. In vitro/ex vivo pharmacological evaluation interfered with an elevated activation of NF-κB and COX-2, increased the type II collagen expression, and inhibited proteoglycan depletion. These results highlight the biocompatibility and the pharmacological efficacy of PL-HA hybrid hydrogels as delivery systems for SFN intra-articular release for OA treatment.
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