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用于治疗脊髓损伤的双重功能支架:壳聚糖膜中载有 sigma 1 受体(S1R)激动剂 RC-33 的海藻酸钠纳米纤维。

Dual-Functioning Scaffolds for the Treatment of Spinal Cord Injury: Alginate Nanofibers Loaded with the Sigma 1 Receptor (S1R) Agonist RC-33 in Chitosan Films.

机构信息

Department of Drug Sciences, University of Pavia, Viale Taramelli, 12, 27100 Pavia, Italy.

Scuola Universitaria IUSS, Istituto Universitario di Studi Superiori, 27100 Pavia, Italy.

出版信息

Mar Drugs. 2019 Dec 26;18(1):21. doi: 10.3390/md18010021.

Abstract

The present work proposed a novel therapeutic platform with both neuroprotective and neuroregenerative potential to be used in the treatment of spinal cord injury (SCI). A dual-functioning scaffold for the delivery of the neuroprotective S1R agonist, RC-33, to be locally implanted at the site of SCI, was developed. RC-33-loaded fibers, containing alginate (ALG) and a mixture of two different grades of poly(ethylene oxide) (PEO), were prepared by electrospinning. After ionotropic cross-linking, fibers were incorporated in chitosan (CS) films to obtain a drug delivery system more flexible, easier to handle, and characterized by a controlled degradation rate. Dialysis equilibrium studies demonstrated that ALG was able to form an interaction product with the cationic RC-33 and to control RC-33 release in the physiological medium. Fibers loaded with RC-33 at the concentration corresponding to 10% of ALG maximum binding capacity were incorporated in films based on CS at two different molecular weights-low (CSL) and medium (CSM)-solubilized in acetic (AA) or glutamic (GA) acid. CSL- based scaffolds were subjected to a degradation test in order to investigate if the different CSL salification could affect the film behavior when in contact with media that mimic SCI environment. CSL AA exhibited a slower biodegradation and a good compatibility towards human neuroblastoma cell line.

摘要

本工作提出了一种具有神经保护和神经再生潜力的新型治疗平台,用于治疗脊髓损伤 (SCI)。开发了一种双重功能支架,用于递送至 SCI 部位的神经保护 S1R 激动剂 RC-33。通过静电纺丝制备了载有 RC-33 的纤维,其中包含海藻酸钠 (ALG) 和两种不同等级的聚环氧乙烷 (PEO) 的混合物。离子交联后,纤维被掺入壳聚糖 (CS) 薄膜中,以获得更灵活、更易于处理且具有受控降解率的药物递送系统。透析平衡研究表明,ALG 能够与阳离子 RC-33 形成相互作用产物,并在生理介质中控制 RC-33 的释放。以两种不同分子量的低 (CSL) 和中 (CSM)-溶解在乙酸 (AA) 或谷氨酸 (GA) 中的方式,将浓度相当于 ALG 最大结合能力 10%的 RC-33 负载纤维掺入 CS 薄膜中。对 CSL 基支架进行了降解测试,以研究不同的 CSL 盐化是否会影响与模拟 SCI 环境的介质接触时的薄膜行为。CSL AA 表现出较慢的生物降解和对人神经母细胞瘤细胞系的良好相容性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f360/7024184/67efc73a1d80/marinedrugs-18-00021-g001.jpg

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