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用于神经再生的载布洛芬聚(碳酸三亚甲基酯-共-ε-己内酯)电纺纤维

Ibuprofen-loaded poly(trimethylene carbonate-co-ε-caprolactone) electrospun fibres for nerve regeneration.

作者信息

Pires Liliana R, Guarino Vincenzo, Oliveira Maria J, Ribeiro Cristina C, Barbosa Mário A, Ambrosio Luigi, Pêgo Ana Paula

机构信息

INEB - Instituto de Engenharia Biomédica, NEWTherapies Group, Universidade do Porto, Porto, Portugal.

Universidade do Porto, Faculdade de Engenharia, Porto, Portugal.

出版信息

J Tissue Eng Regen Med. 2016 Mar;10(3):E154-66. doi: 10.1002/term.1792. Epub 2013 Aug 16.

Abstract

The development of scaffolds that combine the delivery of drugs with the physical support provided by electrospun fibres holds great potential in the field of nerve regeneration. Here it is proposed the incorporation of ibuprofen, a well-known non-steroidal anti-inflammatory drug, in electrospun fibres of the statistical copolymer poly(trimethylene carbonate-co-ε-caprolactone) [P(TMC-CL)] to serve as a drug delivery system to enhance axonal regeneration in the context of a spinal cord lesion, by limiting the inflammatory response. P(TMC-CL) fibres were electrospun from mixtures of dichloromethane (DCM) and dimethylformamide (DMF). The solvent mixture applied influenced fibre morphology, as well as mean fibre diameter, which decreased as the DMF content in solution increased. Ibuprofen-loaded fibres were prepared from P(TMC-CL) solutions containing 5% ibuprofen (w/w of polymer). Increasing drug content to 10% led to jet instability, resulting in the formation of a less homogeneous fibrous mesh. Under the optimized conditions, drug-loading efficiency was above 80%. Confocal Raman mapping showed no preferential distribution of ibuprofen in P(TMC-CL) fibres. Under physiological conditions ibuprofen was released in 24 h. The release process being diffusion-dependent for fibres prepared from DCM solutions, in contrast to fibres prepared from DCM-DMF mixtures where burst release occurred. The biological activity of the drug released was demonstrated using human-derived macrophages. The release of prostaglandin E2 to the cell culture medium was reduced when cells were incubated with ibuprofen-loaded P(TMC-CL) fibres, confirming the biological significance of the drug delivery strategy presented. Overall, this study constitutes an important contribution to the design of a P(TMC-CL)-based nerve conduit with anti-inflammatory properties.

摘要

将药物递送与电纺纤维提供的物理支撑相结合的支架开发在神经再生领域具有巨大潜力。本文提出将一种著名的非甾体抗炎药布洛芬掺入统计共聚物聚(碳酸三亚甲酯 - 共 - ε - 己内酯)[P(TMC - CL)]的电纺纤维中,作为一种药物递送系统,通过限制炎症反应来增强脊髓损伤情况下的轴突再生。P(TMC - CL)纤维由二氯甲烷(DCM)和二甲基甲酰胺(DMF)的混合物电纺而成。所应用的溶剂混合物影响纤维形态以及平均纤维直径,随着溶液中DMF含量的增加,平均纤维直径减小。载布洛芬纤维由含有5%布洛芬(占聚合物重量/重量)的P(TMC - CL)溶液制备。将药物含量增加到10%会导致射流不稳定,从而形成不太均匀的纤维网。在优化条件下,药物负载效率高于80%。共聚焦拉曼映射显示布洛芬在P(TMC - CL)纤维中没有优先分布。在生理条件下,布洛芬在24小时内释放。对于由DCM溶液制备的纤维,释放过程是扩散依赖的,而由DCM - DMF混合物制备的纤维则发生突发释放。使用人源巨噬细胞证明了释放药物的生物活性。当细胞与载布洛芬的P(TMC - CL)纤维一起孵育时,前列腺素E2释放到细胞培养基中的量减少,证实了所提出的药物递送策略的生物学意义。总体而言,这项研究对设计具有抗炎特性的基于P(TMC - CL)的神经导管做出了重要贡献。

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