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圆锥角膜与健康角膜中 aquaporin-5(水通道蛋白 5,AQP5)的表达比较分析

Comparative expression analysis of aquaporin-5 (AQP5) in keratoconic and healthy corneas.

作者信息

Garfias Yonathan, Navas Alejandro, Pérez-Cano Hector J, Quevedo Jonathan, Villalvazo Leonardo, Zenteno Juan Carlos

机构信息

Research Unit, Institute of Ophthalmology Conde de Valenciana, Mexico City, Mexico.

出版信息

Mol Vis. 2008 Apr 25;14:756-61.

Abstract

PURPOSE

Keratoconus (KC) is a common progressive corneal disease characterized by excessive stromal thinning, central or paracentral conical protrusion, and disruptions in Bowman's layer. The etiology of KC is largely unknown, and a combination of genetic and environmental factors is believed to play a role in the origin of the disease. Recently, the absence of transcripts of the water channel, aquaporin-5 (AQP5), was demonstrated by reverse-transcription polymerase chain reaction (RT-PCR) in KC tissues and was proposed as a possible marker for KC. In this study, we sought to evaluate AQP5 mRNA and protein expression in KC and non-KC corneal tissues using a combination of techniques.

METHODS

A total of 69 samples of corneal tissue were analyzed including 39 corneal buttons from patients with advanced KC, 16 samples of non-KC corneal epithelium belonging to patients who underwent surface refractive surgery, 12 sclerocorneal rims obtained from healthy donor subjects, and two healthy corneal buttons. Determination of AQP5 transcript and protein expression patterns was performed by means of real time RT-PCR, immunohistochemistry, immunocytochemistry, and flow cytometry methods. Cell culture was performed to identify AQP5 protein expression in KC epithelial cells.

RESULTS

AQP5 mRNA was expressed with no significant differences between KC and non-KC tissues. Moreover, AQP5 protein expression analysis did not reveal differences in protein levels and/or cell location among KC and non-KC tissues. Interestingly, AQP5 expression continues for up to 21 days in the isolated KC corneal epithelial cells.

CONCLUSIONS

Our results do not support a role for AQP5 in KC etiopathogeny or as a disease marker. Genetic background differences or a distinct pathogenetic KC cascade specific to the analyzed population could account for the dissimilarities observed in KC-related AQP5 expression.

摘要

目的

圆锥角膜(KC)是一种常见的进行性角膜疾病,其特征为基质过度变薄、中央或旁中央圆锥状突出以及Bowman层破坏。KC的病因在很大程度上尚不清楚,人们认为遗传和环境因素的综合作用在该疾病的起源中发挥作用。最近,通过逆转录聚合酶链反应(RT-PCR)在KC组织中证实了水通道蛋白-5(AQP5)水通道的转录本缺失,并被提议作为KC的一种可能标志物。在本研究中,我们试图使用多种技术组合来评估AQP5 mRNA和蛋白在KC和非KC角膜组织中的表达。

方法

共分析了69份角膜组织样本,包括39份来自晚期KC患者的角膜纽扣组织、16份来自接受表面屈光手术患者的非KC角膜上皮样本、12份从健康供体获取的巩膜角膜缘组织以及2份健康角膜纽扣组织。通过实时RT-PCR、免疫组织化学、免疫细胞化学和流式细胞术方法来确定AQP5转录本和蛋白表达模式。进行细胞培养以鉴定KC上皮细胞中AQP5蛋白的表达。

结果

AQP5 mRNA在KC和非KC组织中均有表达,且无显著差异。此外,AQP5蛋白表达分析未揭示KC和非KC组织在蛋白水平和/或细胞定位上的差异。有趣的是,分离的KC角膜上皮细胞中AQP5表达可持续长达21天。

结论

我们的结果不支持AQP5在KC发病机制中起作用或作为疾病标志物。遗传背景差异或所分析人群特有的独特KC致病级联反应可能解释了在KC相关AQP5表达中观察到的差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9b03/2358923/9b7eb8c9ebbf/mv-v14-756-f1.jpg

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