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Transglutaminase binding fusion protein linked to SLPI reduced corneal inflammation and neovascularization

机译:与SLPI连接的转谷氨酰胺酶结合融合蛋白减少了角膜炎症和新血管形成

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摘要

Background: To study the effect of topical administration of a fusion protein (PF-MC) made up of N-terminal portion of the protease inhibitor Trappin-2 (which is a substrate of transglutaminasa-2) and SLPI (protein with anti-inflammatory, anti-bacterial and anti-viral ability), in an animal model of corneal inflammation and angiogenesis. Methods: An alkali injury was produced with a filter paper of 3 mm with 1 N NaOH during 40 seconds on the right cornea of 36 male Sprague Dawley rats, under general anesthesia. Animals were divided into three groups according to treatment. Group 1 was treated with 10 ul of PF-MC (200 ug/ml; n = 12), Group 2, with 10 ul of SLPI (200 ug/ml; n = 12) and Group 3 was treated with buffer (10 ul; n = 12) topically administered four times a day for up to 7 days. Half of the animals were sacrificed at day 3 before making a re-epithelialization time analysis with fluorescein staining at 18 and 24 hours. In the remaining animals corneal opacity was studied and digital photographs were taken at day 7 before doing euthanasia. Eyes were processed for histology and immunofluorescence. Results: Corneal ulcerated area was significantly lower in PF-MC treated animals compared to SLPI and buffer-treated animals at 18 hours and 24 hours postinjury. A clear cornea and fundus red reflex was only found among PF-MC treated animals. Histological analysis revealed a stratified corneal epithelium with at least three layers in all PF-MC animals at day 7. In this group there was a reduced number of PMNs in the corneal stroma at 3 and 7 days of follow-up. Besides, corneal neovascularization was much more extended in SLPI and Buffer animals than in animals treated with PF-MC. Conclusions: The binding of SLPI with Cementoin to transglutaminase seems to be an effective strategy to treat corneal inflammation and angiogenesis.
机译:背景:研究局部施用由蛋白酶抑制剂Trappin-2(是转谷氨酰胺酶2的底物)和SLPI(具有抗炎作用的蛋白)的N端部分组成的融合蛋白(PF-MC)的局部给药效果,抗细菌和抗病毒能力)在角膜炎症和血管生成的动物模型中发挥作用。方法:在全麻下,在36 s Sprague Dawley雄性大鼠的右角膜上,用3μmm的滤纸和1 N的NaOH在40秒钟内对3mm的碱膜造成碱损伤。根据治疗将动物分为三组。第1组用10 ul PF-MC(200 ug / ml; n = 12)处理,第2组用10 ul SLPI(200 ug / ml; n = 12)处理,第3组用缓冲液(10 ul)处理; n = 12)每天局部给药四次,最多7天。在第3天处死一半动物,然后在18和24小时时用荧光素染色进行重新上皮化时间分析。在其余动物中,研究了角膜混浊并在进行安乐死之前的第7天拍摄了数码照片。对眼睛进行组织学和免疫荧光处理。结果:在损伤后18小时和24小时,PF-MC处理的动物的角膜溃疡面积显着低于SLPI和缓冲液处理的动物。仅在PF-MC治疗的动物中发现了清晰的角膜和眼底红反射。组织学分析显示,在第7天,所有PF-MC动物的分层角膜上皮至少有三层。在此组中,随访3天和7天,角膜基质中的PMN数量减少。此外,与用PF-MC治疗的动物相比,SLPI和Buffer动物的角膜新血管形成更加广泛。结论:SLPI与骨水泥结合到转谷氨酰胺酶似乎是治疗角膜炎症和血管生成的有效策略。

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