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蛋白质聚合物纳米颗粒介导的拉科立丁促进角膜上皮再生

Lacritin-mediated regeneration of the corneal epithelia by protein polymer nanoparticles.

作者信息

Wang Wan, Despanie Jordan, Shi Pu, Edman-Woolcott Maria C, Lin Yi-An, Cui Honggang, Heur J Martin, Fini M Elizabeth, Hamm-Alvarez Sarah F, MacKay J Andrew

机构信息

Department of Pharmacology and Pharmaceutical Sciences, University of Southern California Los Angeles, CA; 90033-9121.

Department of Chemical and Biomolecular Engineering, Johns Hopkins University, Baltimore, MD; 21218.

出版信息

J Mater Chem B. 2014 Dec 14;2(46):8131-8141. doi: 10.1039/C4TB00979G.

Abstract

The avascular corneal epithelium plays an important role in maintaining normal vision and protecting the corneal interior from environmental infections. Delayed recovery of ocular wounds caused by trauma or refractive surgery strengthens the need to accelerate corneal wound healing and better restore the ocular surface. To address this need, we fused elastin-like polypeptide (ELP) based nanoparticles SI with a model mitogenic protein called lacritin. Lacritin fused at the N-terminus of the SI diblock copolymer is called LSI. This LSI fusion protein undergoes thermo-responsive assembly of nanoparticles at physiologically relevant temperatures. In comparison to ELP nanoparticles without lacritin, LSI showed potent signs of lacritin specific effects on a human corneal epithelial cell line (HCE-T), which included enhancement of cellular uptake, calcium-mediated signaling, and closure of a scratch. , the corneas of non-obese diabetic mice (NOD) were found to be highly responsive to LSI. Fluorescein imaging and corneal histology suggested that topical administration of LSI onto the ocular surface significantly promoted corneal wound healing and epithelial integrity compared to mice treated with or without plain ELP. Most interestingly, it appears that ELP-mediated assembly of LSI is essential to produce this potent activity. This was confirmed by comparison to a control lacritin ELP fusion called LS96, which does not undergo thermally-mediated assembly at relevant temperatures. In summary, fusion of a mitogenic protein to ELP nanoparticles appears to be a promising new strategy to bioengineer more potent biopharmaceuticals with potential applications in corneal wound healing.

摘要

无血管的角膜上皮在维持正常视力以及保护角膜内部免受环境感染方面发挥着重要作用。创伤或屈光手术导致的眼外伤愈合延迟,强化了加速角膜伤口愈合以及更好地恢复眼表的需求。为满足这一需求,我们将基于弹性蛋白样多肽(ELP)的纳米颗粒SI与一种名为拉克立丁的促有丝分裂蛋白模型进行了融合。在SI二嵌段共聚物的N端融合了拉克立丁的产物被称为LSI。这种LSI融合蛋白在生理相关温度下会发生纳米颗粒的热响应组装。与不含拉克立丁的ELP纳米颗粒相比,LSI在人角膜上皮细胞系(HCE-T)上表现出拉克立丁特异性效应的显著迹象,其中包括细胞摄取增强、钙介导的信号传导以及划痕闭合。此外,发现非肥胖糖尿病小鼠(NOD)的角膜对LSI高度敏感。荧光素成像和角膜组织学表明,与用普通ELP处理或未处理的小鼠相比,在眼表局部应用LSI可显著促进角膜伤口愈合和上皮完整性。最有趣的是,ELP介导的LSI组装似乎对于产生这种强效活性至关重要。与一种名为LS96的对照拉克立丁ELP融合物相比证实了这一点,LS96在相关温度下不会发生热介导的组装。总之,将促有丝分裂蛋白与ELP纳米颗粒融合似乎是一种有前景的新策略,可用于生物工程更有效的生物药物,在角膜伤口愈合方面具有潜在应用。

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