RPE-secreted factors: influence differentiation in human retinal cell line in dose- and density-dependent manner.

Kamla Dutt, Paul Douglas, Yang Cao
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引用次数: 12

Abstract

Retinal pigment epithelial (RPE) cells play an important role in normal functioning of retina and photoreceptors, and some retinal degenerations arise due to malfunctioning RPE. Retinal pigment epithelium transplantation is being explored as a strategy to rescue degenerating photoreceptors in diseases such as age-related macular degeneration (AMD) and retinitis pigmentosa (RP). Additionally, RPE-secreted factors could rescue degenerating photoreceptors by prolonging survival or by their ability to differentiate and give rise to photoreceptors by transdifferentiation. In this study, we have explored what role cell density could play in differentiation induced in a human retinal progenitor cell line, in response to RPE-secreted growth factors. Retinal progenitors plated at low (1 × 10(4) cells/cm(2)), medium (2-4 × 10(4) cells/cm(2)), and high (1 × 10(5) cells/cm(2)) cell density were exposed to various dilutions of RPE-conditioned medium (secreted factors) under conditions of defined medium culture. Progenitor cell differentiation was monitored phenotypically (morphological, biochemical analysis, and immunophenotyping, and western blot analysis were performed). Our data show that differentiation in response to RPE-secreted factors is modulated by cell density and dilutions of conditioned medium. We conclude that before embarking on RPE transplantation as a modality for treatment of RP and AMD, one will have to determine the role that cell density and inhibitory and stimulatory neurotrophins secreted by RPE could play in the efficacy of survival of transplants. We report that RPE-conditioned medium enhances neuronal phenotype (photoreceptors, bipolars) at the lowest cell density in the absence of cell-cell contact. Eighty percent to 90% of progenitor cells differentiate into photoreceptors and bipolars at 50% concentration of conditioned medium, while exposure to 100% conditioned medium might increase multipolar neurons (ganglionic and amacrine phenotypes) to a small degree. However, no clear-cut pattern of differentiation in response to RPE-secreted factors is noted at higher cell densities.

rpe分泌因子:以剂量和密度依赖的方式影响人视网膜细胞系的分化。
视网膜色素上皮细胞(RPE)在视网膜和光感受器的正常功能中起着重要作用,一些视网膜变性是由于RPE功能异常引起的。视网膜色素上皮移植正在被探索作为一种策略来拯救退化的光感受器疾病,如年龄相关性黄斑变性(AMD)和色素性视网膜炎(RP)。此外,rpe分泌因子可以通过延长存活时间或通过转分化分化产生光感受器来挽救退化的光感受器。在这项研究中,我们探索了细胞密度在rpe分泌的生长因子诱导的人视网膜祖细胞系分化中所起的作用。低(1 × 10(4)个细胞/cm(2))、中(2-4 × 10(4)个细胞/cm(2))和高(1 × 10(5)个细胞/cm(2))细胞密度的视网膜祖细胞,在规定的培养基培养条件下,暴露于不同稀释度的rpe条件培养基(分泌因子)中。对祖细胞分化进行表型监测(形态学、生化分析、免疫表型分析和western blot分析)。我们的数据表明,rpe分泌因子的分化反应受细胞密度和条件培养基稀释度的调节。我们的结论是,在将RPE移植作为治疗RP和AMD的一种方式之前,我们必须确定RPE分泌的细胞密度和抑动性和刺激性神经营养因子在移植存活的疗效中所起的作用。我们报告说,rpe条件培养基在细胞密度最低的情况下,在没有细胞间接触的情况下,增强神经元表型(光感受器,双极)。在条件培养基浓度为50%时,80% - 90%的祖细胞分化为光感受器和双极细胞,而暴露于100%条件培养基可能会在一定程度上增加多极神经元(神经节和无毛细胞表型)。然而,在较高的细胞密度下,没有明确的分化模式响应rpe分泌因子。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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