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地塞米松和贝伐单抗组成的超分子水凝胶通过抑制炎症反应减轻大鼠碱烧伤角膜新生血管化。

Combination of dexamethasone and Avastin by supramolecular hydrogel attenuates the inflammatory corneal neovascularization in rat alkali burn model.

机构信息

School of Ophthalmology & Optometry and Eye Hospital, Wenzhou Medical University, 270 Xueyuan Road, Wenzhou, 325035, PR China.

Institute of Biomaterials and Engineering, Wenzhou Medical University, Wenzhou, 325035, PR China.

出版信息

Colloids Surf B Biointerfaces. 2017 Nov 1;159:241-250. doi: 10.1016/j.colsurfb.2017.07.057. Epub 2017 Jul 25.

DOI:10.1016/j.colsurfb.2017.07.057
PMID:28800463
Abstract

Corneal neovascularization (CNV) is one of the leading causes of vision loss and a high-risk factor for transplant rejection. The present study proposed a supramolecular hydrogel comprised of MPEG-PCL micelles and α-cyclodextrin (α-CD) for co-delivery of dexamethasone sodium phosphate (Dexp) and Avastin (Ava), and further evaluated its therapeutic efficacy in rat alkali burn model. A physical mixing of Dexp/Ava, MPEG-PCL micelles, and α-CD aqueous solution leads to a spontaneous formation of the supramolecular hydrogel via a "host-guest" recognition between MPEG and α-CD. The supramolecular hydrogel provides a relatively quick release of Dexp over Ava during the study of the 5-day in vitro release. The results of in vitro cytotoxicity test and wound healing assay illustrated that the proposed supramolecular hydrogel was non-toxic against L-929 and HCEC cells and did not significantly affect the migration of HCEC cells after 24h incubation. The corneal distribution test suggested that the precorneal duration of Ava was significantly extended by the supramolecular hydrogel with respect to its solution formulation. Moreover, the supramolecular hydrogel showed high ocular biocompatibility and was a non-irritant after topical instillation. Furthermore, the Dexp-Ava hydrogel medication, but not by Ava solution and Ava hydrogel medication, could greatly attenuate the alkali burn-induced corneal inflammation and remarkably suppress the corneal neovascularization via the downregulation of VEGF, CD31, and α-SMA expression in the rat alkali burn model. As a result, the combined Dexp and Ava by supramolecular hydrogel exhibited an advantage over Ava monotherapy approach, which might be a promising alternative therapy for inflammatory CNV.

摘要

角膜新生血管(CNV)是导致视力丧失的主要原因之一,也是移植排斥的高危因素。本研究提出了一种由 MPEG-PCL 胶束和α-环糊精(α-CD)组成的超分子水凝胶,用于共递送地塞米松磷酸钠(Dexp)和阿瓦斯汀(Ava),并进一步评估了其在大鼠碱烧伤模型中的治疗效果。Dexp/Ava、MPEG-PCL 胶束和α-CD 水溶液的物理混合导致通过 MPEG 和α-CD 之间的“主客体”识别自发形成超分子水凝胶。在 5 天的体外释放研究中,超分子水凝胶提供了相对快速释放 Dexp 而不是 Ava。体外细胞毒性试验和伤口愈合试验的结果表明,所提出的超分子水凝胶对 L-929 和 HCEC 细胞无毒性,并且在 24 小时孵育后对 HCEC 细胞的迁移没有显著影响。角膜分布试验表明,与溶液制剂相比,超分子水凝胶显著延长了 Ava 的预角膜持续时间。此外,超分子水凝胶具有高眼生物相容性,经局部滴注后无刺激性。此外,Dexp-Ava 水凝胶给药,而不是 Ava 溶液和 Ava 水凝胶给药,可通过下调大鼠碱烧伤模型中 VEGF、CD31 和α-SMA 的表达,显著减轻碱烧伤引起的角膜炎症,并显著抑制角膜新生血管形成。因此,超分子水凝胶联合 Dexp 和 Ava 比 Ava 单药治疗具有优势,可能是一种有前途的炎症性 CNV 替代治疗方法。

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