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Characterisation of the advanced glycation endproduct receptor complex in the retinal pigment epithelium

机译:视网膜色素上皮中晚期糖基化终产物受体复合物的表征

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>Aims: Advanced glycation endproducts (AGEs) accumulate with ageing and may have a significant impact on age related dysfunction of the retinal pigment epithelium (RPE). Many of the cellular effects of AGEs in other cell types are mediated through AGE binding proteins. The aim of this study was to characterise the AGE receptor complex in RPE cells in vitro and to focus on the role of the R3 component (galectin-3) as the primary effector of the complex.>Methods: Primary cultures of bovine RPE cells and the human D407 RPE cell line were exposed to AGE modified albumin. Receptor expression was determined using mRNA analysis by quantitative real time RT-PCR and protein characterisation by western blotting. Immunocytochemical analysis examined the cellular localisation of the various components of the AGE receptor complex. The role of the galectin-3 receptor component was examined by transfection and overexpression using the D407 cell line and analysis of soluble AGE-R3 by ELISA.>Results: All three components of the AGE receptor complex were expressed by bovine and human RPE cells. AGE exposure upregulated two components of the receptor complex and also induced significant RPE expression of VEGF mRNA (p<0.05). RPE D407 cells stably transfected to overexpress galectin-3 showed less VEGF induction. In non-transfected RPE which were exposed to AGEs, there was less soluble galectin-3 protein released into the medium (p<0.05), a response that was not evident in transfected cells.>Conclusion: A conserved AGE receptor complex is evident in primary cultures of bovine RPE cells and also in a human cell line. These cells show a pathological response to AGE exposure, an effect which appears to be modulated by the galectin-3 component of the receptor complex.
机译:>目的:随着年龄的增长,晚期糖基化终产物(AGEs)会累积,并可能对与年龄有关的视网膜色素上皮(RPE)功能障碍产生重大影响。 AGEs在其他细胞类型中的许多细胞作用是通过AGE结合蛋白介导的。这项研究的目的是在体外表征RPE细胞中的AGE受体复合物,并着重研究R3成分(galectin-3)作为该复合物的主要效应物的作用。>方法:牛RPE细胞和人D407 RPE细胞系的培养物暴露于AGE修饰的白蛋白。受体表达通过定量实时RT-PCR使用mRNA分析确定,并通过蛋白质印迹法进行蛋白质表征。免疫细胞化学分析检查了AGE受体复合物各种成分的细胞定位。通过使用D407细胞系转染和过表达并通过ELISA分析可溶性AGE-R3来检验galectin-3受体组分的作用。>结果:牛和人的RPE细胞。 AGE暴露上调了受体复合物的两个成分,并且还诱导了VEGF mRNA的显着RPE表达(p <0.05)。稳定转染过表达Rect D-3的RPE D407细胞显示出较少的VEGF诱导作用。在暴露于AGEs的未转染的RPE中,可溶性半乳凝素3蛋白释放到培养基中的数量较少(p <0.05),这种反应在转染的细胞中不明显。>结论: AGE受体复合物在牛RPE细胞的原代培养物中以及在人类细胞系中都很明显。这些细胞表现出对AGE暴露的病理反应,这种作用似乎由受体复合物的半乳凝素3组分调节。

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