Effect of Periplaneta americana Extract on Corneal Fibrosis and Epithelial Healing After Rabbit Lamellar Keratectomy.

IF 2.6 3区 医学 Q2 OPHTHALMOLOGY
Yijing Li, Liting Zhu, Zheng Yuan, Chunyang Zhou
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引用次数: 0

Abstract

Purpose: To evaluate Periplaneta americana extract (PAE) effects on corneal epithelial healing and fibrosis after superficial lamellar keratectomy (SLK) in rabbits.

Methods: SLK was performed on the right eyes of 48 New Zealand White rabbits, randomized into three treatment groups (n = 16/group): normal saline (NS), Tobradex eye drops (TE), and PAE group. Corneal opacity and epithelial defect area were quantified using slit-lamp imaging at postoperative days 3, 7, 14, and 28 (D3, D7, D14, and D28) and scored via the grading system. We performed histopathological analysis to visualize tissue structure and immunohistochemistry (IHC) localize and quantify TGF-β1 protein in corneal tissues.

Results: Significant intergroup differences in corneal epithelial defect area and opacity were observed on D3 and D7 (all P < 0.05). The TE group exhibited the largest epithelial defects but mildest corneal opacity, whereas the PAE group demonstrated the smallest epithelial defects and significantly reduced opacity compared to the NS group (P < 0.05). Time-dependent variations in epithelial defect area were noted across all groups (P < 0.05). The NS and TE groups displayed progressive corneal opacity increases, whereas the opacity of the PAE group peaked at D7 before declining. Histological analysis revealed epithelial detachment, stromal edema, and inflammatory infiltration in all groups, with the TE group showing milder inflammation. TGF-β1 expression levels initially increased followed by a decline in the NS and PAE groups, in contrast to the inverse trend of the TE group. No statistically significant differences in late-phase corneal opacity or TGF-β1 levels were observed between groups (all P > 0.05).

Conclusions: During the early phase after SLK, PAE accelerated corneal tissue regeneration, inhibited corneal scarring, and partially restored corneal clarity. This biphasic regulatory effect may be attributed to promoting TGF-β1 expression in the early stage, followed by its inhibition in the later stages.

Translational relevance: PAE modulates TGF-β1 to balance corneal healing and fibrosis as a novel topical corticosteroid alternative, warranting human trials for its dual-phase healing/scarring action.

美洲大蠊提取物对兔板层角膜切除术后角膜纤维化及上皮愈合的影响。
目的:探讨美洲大蠊提取物(PAE)对兔浅板层角膜切除术(SLK)后角膜上皮愈合及纤维化的影响。方法:48只新西兰大白兔右眼行SLK治疗,随机分为生理盐水组(NS)、托布莱德滴眼液组(TE)和PAE组(n = 16/组)。术后第3、7、14和28天(D3、D7、D14和D28)采用裂隙灯成像对角膜不透明和上皮缺损面积进行量化,并通过分级系统进行评分。我们进行组织病理学分析,可视化组织结构,免疫组化(IHC)定位和定量角膜组织中TGF-β1蛋白。结果:D3、D7组间角膜上皮缺损面积、混浊度差异均有统计学意义(P < 0.05)。TE组上皮缺损最大,角膜混浊最轻,而PAE组上皮缺损最小,角膜混浊较NS组显著降低(P < 0.05)。各组上皮缺损面积随时间变化(P < 0.05)。NS组和TE组角膜混浊逐渐增加,PAE组角膜混浊在D7时达到峰值后逐渐下降。组织学分析显示各组上皮脱离、间质水肿、炎症浸润,TE组炎症较轻。TGF-β1表达水平在NS组和PAE组呈先升高后下降的趋势,与TE组相反。各组间晚期角膜混浊、TGF-β1水平差异均无统计学意义(P < 0.05)。结论:在SLK术后早期,PAE可加速角膜组织再生,抑制角膜瘢痕形成,部分恢复角膜清晰度。这种双相调节作用可能是早期促进TGF-β1表达,后期抑制TGF-β1表达。翻译相关性:PAE调节TGF-β1以平衡角膜愈合和纤维化,作为一种新的外用皮质类固醇替代品,需要对其双阶段愈合/疤痕作用进行人体试验。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Translational Vision Science & Technology
Translational Vision Science & Technology Engineering-Biomedical Engineering
CiteScore
5.70
自引率
3.30%
发文量
346
审稿时长
25 weeks
期刊介绍: Translational Vision Science & Technology (TVST), an official journal of the Association for Research in Vision and Ophthalmology (ARVO), an international organization whose purpose is to advance research worldwide into understanding the visual system and preventing, treating and curing its disorders, is an online, open access, peer-reviewed journal emphasizing multidisciplinary research that bridges the gap between basic research and clinical care. A highly qualified and diverse group of Associate Editors and Editorial Board Members is led by Editor-in-Chief Marco Zarbin, MD, PhD, FARVO. The journal covers a broad spectrum of work, including but not limited to: Applications of stem cell technology for regenerative medicine, Development of new animal models of human diseases, Tissue bioengineering, Chemical engineering to improve virus-based gene delivery, Nanotechnology for drug delivery, Design and synthesis of artificial extracellular matrices, Development of a true microsurgical operating environment, Refining data analysis algorithms to improve in vivo imaging technology, Results of Phase 1 clinical trials, Reverse translational ("bedside to bench") research. TVST seeks manuscripts from scientists and clinicians with diverse backgrounds ranging from basic chemistry to ophthalmic surgery that will advance or change the way we understand and/or treat vision-threatening diseases. TVST encourages the use of color, multimedia, hyperlinks, program code and other digital enhancements.
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