Controlled local release of PPARγ agonists from biomaterials to treat peripheral nerve injury

医学 再生(生物学) 药物输送 布洛芬 坐骨神经 控制释放 神经损伤 药理学 周围神经 药品 生物医学工程 麻醉 化学 解剖 有机化学 生物 细胞生物学
作者
Melissa Rayner,Alessandra Grillo,Gareth R. Williams,Essam A. Tawfik,T Zhang,Charitini Volitaki,Duncan Q.M. Craig,Jess Healy,James B. Phillips
出处
期刊:Journal of Neural Engineering [IOP Publishing]
卷期号:17 (4): 046030-046030 被引量:20
标识
DOI:10.1088/1741-2552/aba7cc
摘要

Abstract Objective. Poor clinical outcomes following peripheral nerve injury (PNI) are partly attributable to the limited rate of neuronal regeneration. Despite numerous potential drug candidates demonstrating positive effects on nerve regeneration rate in preclinical models, no drugs are routinely used to improve restoration of function in clinical practice. A key challenge associated with clinical adoption of drug treatments in nerve injured patients is the requirement for sustained administration of doses associated with undesirable systemic sideeffects. Local controlled-release drug delivery systems could potentially address this challenge, particularly through the use of biomaterials that can be implanted at the repair site during the microsurgical repair procedure. Approach. In order to test this concept, this study used various biomaterials to deliver ibuprofen sodium or sulindac sulfide locally in a controlled manner in a rat sciatic nerve injury model. Following characterisation of release parameters in vitro , ethylene vinyl acetate tubes or polylactic-co-glycolic acid wraps, loaded with ibuprofen sodium or sulindac sulfide, were placed around directly-repaired nerve transection or nerve crush injuries in rats. Main results. Ibuprofen sodium, but not sulindac sulfide caused an increase in neurites in distal nerve segments and improvements in functional recovery in comparison to controls with no drug treatment. Significance. This study showed for the first time that local delivery of ibuprofen sodium using biomaterials improves neurite growth and functional recovery following PNI and provides the basis for future development of drug-loaded biomaterials suitable for clinical translation.
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