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组织工程法生成的 NANOULCOR 纳米结构纤维蛋白-琼脂糖人角膜替代物的组织学、组织化学和免疫组织化学特性。

Histological, histochemical, and immunohistochemical characterization of NANOULCOR nanostructured fibrin-agarose human cornea substitutes generated by tissue engineering.

机构信息

Department of Histology, Tissue Engineering Group, School of Medicine, University of Granada, Granada, Spain.

Instituto de Investigación Biosanitaria ibs.GRANADA, Granada, Spain.

出版信息

BMC Med. 2024 Nov 13;22(1):531. doi: 10.1186/s12916-024-03759-4.

Abstract

BACKGROUND

Human artificial corneas (HAC) generated by tissue engineering recently demonstrated clinical usefulness in the management of complex corneal diseases. However, the biological mechanisms associated to their regenerative potential need to be elucidated.

METHODS

In the present work, we generated HAC using nanostructured fibrin-agarose biomaterials with cultured corneal epithelial and stromal cells, and we compared the structure and histochemical and immunohistochemical profiles of HAC with control native corneas (CTR-C) and limbus (CTR-L) to determine the level of biomimicry of the HAC with these two native organs.

RESULTS

HAC tissues consisted of a stratified epithelium and a cellular stromal substitute. The interface between stroma and epithelium was similar to that of CTR-C, without the finger-shaped palisades of Vogt found in CTR-L, and contained a poorly developed basement membrane as determined by PAS histochemistry. Analysis of the stromal layer revealed that HAC contained significantly lower amounts of extracellular matrix components (collagen, proteoglycans, decorin, keratocan, and lumican) than CTR-C and CTR-L, with all samples being devoid of elastic and reticular fibers. At the epithelial level, HAC were strongly positive for several cytokeratins, although KRT5 was lower in HAC as compared to CTR-C and CTR-L. The expression of crystallin lambda was lower in HAC than in control tissues, whereas crystallin alpha-a was similar in HAC and CTR-C. No differences were found among HAC and controls for the cell-cell junction proteins CX43 and TJP1. When specific markers were analyzed, we found that HAC expression profile of KRT3, KRT19, KRT15, and ΔNp63 was more similar to CTR-L than to CTR-C.

CONCLUSIONS

These results suggest that HAC generated in the laboratory could be structurally and functionally more biomimetic to the structure found at the corneal limbus than to the central cornea, and open the door to the use of these artificial tissues in patients with limbal deficiency.

摘要

背景

组织工程生成的人人工角膜(HAC)最近在复杂角膜疾病的治疗中显示出临床应用价值。然而,其再生潜能相关的生物学机制仍需要阐明。

方法

在本研究中,我们使用纳米结构纤维蛋白-琼脂糖生物材料,培养角膜上皮和基质细胞,生成 HAC,并将其与对照天然角膜(CTR-C)和角膜缘(CTR-L)的结构、组织化学和免疫组织化学特征进行比较,以确定 HAC 与这两种天然器官的仿生程度。

结果

HAC 组织由分层上皮和细胞基质替代物组成。基质和上皮之间的界面类似于 CTR-C,没有在 CTR-L 中发现的 Vogt 指状嵴,通过 PAS 组织化学分析发现,基底膜发育不良。对基质层的分析表明,HAC 中细胞外基质成分(胶原蛋白、蛋白聚糖、decorin、keratocan 和 lumican)的含量明显低于 CTR-C 和 CTR-L,所有样本均缺乏弹性纤维和网状纤维。在上皮层,HAC 对几种细胞角蛋白呈强阳性,尽管 HAC 中的 KRT5 低于 CTR-C 和 CTR-L。与对照组织相比,HAC 中的晶状体 lambda 表达水平较低,而 HAC 中的晶状体 alpha-a 与 CTR-C 相似。HAC 和对照组织之间在细胞间连接蛋白 CX43 和 TJP1 方面没有差异。当分析特定标志物时,我们发现 HAC 的 KRT3、KRT19、KRT15 和 ΔNp63 表达谱与 CTR-L 更相似,而与 CTR-C 不相似。

结论

这些结果表明,在实验室中生成的 HAC 在结构上和功能上可能更仿生于角膜缘的结构,而不是中央角膜,为这些人工组织在角膜缘缺陷患者中的应用开辟了道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f7f0/11562680/d7c45398d52b/12916_2024_3759_Fig1_HTML.jpg

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