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首页> 外文期刊>Experimental Eye Research >Differential response of lens crystallins and corneal crystallins in degenerative corneas
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Differential response of lens crystallins and corneal crystallins in degenerative corneas

机译:晶状体晶状体蛋白和角膜晶状体蛋白在变性角膜中的差异反应

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摘要

Corneal degenerations, occurring either spontaneously or as a complication to other diseases, cause vision problems by endangering corneal transparency. Our past cornea research projects involving mice revealed that some recruited mice presented corneal problems similar to human corneal degeneration. The present study examines the histology of diseased mice corneas, including ultrastructure. Genome-wide microarray and proteomic methods were utilized to screen for molecular changes in the diseased corneas. It was found that abnormalities affected mainly anterior layers of the corneas. The most often observed histological abnormalities included neoplasm or detachment of the epithelial layer, erosion or breakage of Bowman membranes, blood vessel formation, and bleeding in the stroma. Microarray assay showed that among the 46 up-regulated probes in diseased corneas, 13 were for lens crystallins. However, all corneal crystallins genes remained unchanged. αA-crystallin was among the proteins that showed the greatest increase in diseased corneas, as detected by gel electrophoresis. We propose that lens crystallins, rather than corneal crystallins, are involved in the pathological process of corneal degeneration. Further study along these lines would provide insight into the mechanism of corneal transparency.
机译:自然发生或与其他疾病并发的角膜变性会危及角膜透明性,从而引起视力问题。我们过去涉及小鼠的角膜研究项目表明,一些新招募的小鼠出现了类似于人角膜变性的角膜问题。本研究检查了病变小鼠角膜的组织学,包括超微结构。全基因组微阵列和蛋白质组学方法被用来筛选患病角膜的分子变化。发现异常主要影响角膜的前层。最常观察到的组织学异常包括肿瘤或上皮层脱离,鲍曼膜的糜烂或破裂,血管形成和基质出血。微阵列分析显示,在患病角膜的46种上调探针中,有13种是晶状体晶状体蛋白。但是,所有角膜结晶蛋白基因均保持不变。通过凝胶电泳检测,αA-晶状体蛋白是显示患病角膜增加最大的蛋白质之一。我们提出晶状体晶状体蛋白,而不是角膜晶状体蛋白,参与角膜变性的病理过程。沿着这些思路进行进一步的研究将有助于深入了解角膜透明性的机制。

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