An in vitro pre-screening model to evaluate the corneal anti-inflammatory effect of human blood-derived products and amniotic membrane extracts incorporated into gelatine-based hydrogels

IF 2.7 2区医学 Q1 OPHTHALMOLOGY

Experimental eye research Pub Date : 2025-08-30 DOI:10.1016/j.exer.2025.110617

Cristina Romo-Valera , Jaime Etxebarria , Vanesa Freire , Juan Durán de la Colina , Jon Arluzea , Noelia Andollo

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Abstract

The objective of this study was to develop a reliable, cost-effective, and rapid in vitro model employing real-time PCR to assess inflammatory responses in hydrogel-based systems, and to comparatively evaluate the anti-inflammatory efficacy of human serum (HS), serum derived from plasma rich in growth factors (sPRGF), and human amniotic membrane extracts (HAMe) incorporated into gelatin-based hydrogels. An in vitro model of corneal inflammation was established by quantifying IL-1β expression via qPCR in TNFα-stimulated SV-40 immortalised human corneal epithelial (HCE) cells. Hydrogels functionalised with HS, sPRGF, or HAMe sourced from proximal, medial, distal, or pooled amniotic regions were evaluated for their anti-inflammatory potential. In vivo validation was conducted in a rabbit anterior stromal keratectomy model, assessing epithelial wound closure and clinical signs of irritation following application of unmodified hydrogels or hydrogels functionalised with autologous serum (AS) or HAMe. In vitro, hydrogels incorporating HS, followed by sPRGF and pooled HAMe, significantly attenuated IL-1β expression, whereas unmodified hydrogels exacerbated the inflammatory response; region-specific HAMe hydrogels demonstrated inconsistent effects. In vivo, AS-functionalised hydrogels facilitated complete re-epithelialisation by day 7 and achieved the lowest irritation scores, indicating both therapeutic efficacy and high tolerability. All hydrogel formulations were found to be biocompatible throughout the study period. These findings underscore the significant anti-inflammatory and regenerative potential of gelatin-based hydrogels functionalised with blood-derived products and support their development as bioactive platforms for ocular surface therapy. Furthermore, the in vitro model provides a robust preclinical screening tool, contributing to the refinement and reduction of animal use in biomedical research.

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建立体外预筛选模型，评价人血源性产品和羊膜提取物掺入明胶基水凝胶的角膜抗炎作用

本研究的目的是建立一种可靠、经济、快速的体外模型，采用实时荧光定量PCR技术评估水凝胶体系中的炎症反应，并比较评价明胶基水凝胶中人血清（HS）、富生长因子血浆衍生血清（sPRGF）和人羊膜提取物（HAMe）的抗炎功效。采用qPCR定量检测tnf α刺激的SV-40永生化人角膜上皮（HCE）细胞IL-1β的表达，建立角膜炎症模型。用近端、中端、远端或汇集羊膜区域的HS、sPRGF或HAMe功能化的水凝胶评估其抗炎潜力。在兔前间质角膜切除术模型中进行了体内验证，评估未修饰水凝胶或用自体血清（AS）或HAMe功能化的水凝胶应用后上皮伤口愈合和临床刺激症状。在体外，加入HS、sPRGF和混合HAMe的水凝胶显著降低了IL-1β的表达，而未修饰的水凝胶则加重了炎症反应；区域特异性HAMe水凝胶表现出不一致的效果。在体内，as功能化的水凝胶在第7天促进了完全的再上皮化，并且达到了最低的刺激评分，表明了治疗效果和高耐受性。在整个研究期间，所有水凝胶制剂均具有生物相容性。这些发现强调了明胶基水凝胶具有显著的抗炎和再生潜力，并支持其作为眼表治疗的生物活性平台的发展。此外，体外模型提供了一个强大的临床前筛选工具，有助于改进和减少生物医学研究中的动物使用。

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来源期刊

Experimental eye research 医学-眼科学

CiteScore

6.80

自引率

5.90%

发文量

323

审稿时长

66 days

期刊介绍： The primary goal of Experimental Eye Research is to publish original research papers on all aspects of experimental biology of the eye and ocular tissues that seek to define the mechanisms of normal function and/or disease. Studies of ocular tissues that encompass the disciplines of cell biology, developmental biology, genetics, molecular biology, physiology, biochemistry, biophysics, immunology or microbiology are most welcomed. Manuscripts that are purely clinical or in a surgical area of ophthalmology are not appropriate for submission to Experimental Eye Research and if received will be returned without review.