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A cell culture condition that induces the mesenchymal-epithelial transition of dedifferentiated porcine retinal pigment epithelial cells

机译:一种细胞培养条件,诱导消化不良猪视网膜色素上皮细胞的间充质 - 上皮转变

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摘要

The pathological change of retinal pigment epithelial (RPE) cells is one of the main reasons for the development of age-related macular degeneration (AMD). Thus, cultured RPE cells are a proper cell model for studying the etiology of AMD in vitro. However, such cultured RPE cells easily undergo epithelial-mesenchymal transition (EMT) that results in changes of cellular morphology and functions of the cells. To restore and maintain the mesenchymal-epithelial transition (MET) of the cultured RPE cells, we cultivated dedifferentiated porcine RPE (pRPE) cells and compared their behaviors in four conditions: 1) in cell culture dishes with DMEM/F12 containing FBS (CC dish-FBS), 2) in petri dishes with DMEM/F12 containing FBS (Petri dish-FBS), 3) in cell culture dishes with DMEM/F12 containing N2 and B27 supplements (CC dish-N2B27), and 4) in petri dishes with DMEM/F12 containing N2 and B27 (Petri dish-N2B27). In addition to observing the cell morphology and behavior, RPE specific markers, as well as EMT-related genes and proteins, were examined by immunostaining, quantitative real-time PCR and Western blotting. The results showed that dedifferentiated pRPE cells maintained EMT in CC dish-FBS, Petri dish-FBS and CC dish-N2B27 groups, whereas MET was induced when the dedifferentiated pRPE cells were cultured in Petri dish-N2B27. Such induced pRPE cells showed polygonal morphology with increased expression of RPE-specific markers and decreased EMT-associated markers. Similar results were observed in induced pluripotent stem cell-derived RPE cells. Furthermore, during the re-differentiation of those dedifferentiated pRPE cells, Petri dish-N2B27 reduced the activity of RhoA and induced F-actin rearrangement, which promoted the nuclear exclusion of transcriptional co-activator with PDZ-binding motif (TAZ) and TAZ target molecule zinc finger E-box binding protein (ZEB1), both of which are EMT inducing factors. This study provides a simple and reliable method to reverse dedifferentiated phenotype of pRPE cells into epithelialized phenotype, which is more appropriate for studying AMD in vitro, and suggests that MET of other cell types might be induced by a similar approach.
机译:视网膜颜料上皮(RPE)细胞的病理变化是年龄相关性黄斑变性(AMD)的主要原因之一。因此,培养的RPE细胞是用于研究体外AMD的病因的适当细胞模型。然而,这种培养的RPE细胞容易经过上皮 - 间充质转换(EMT),导致细胞形态和细胞功能的变化。为了恢复和维持培养的RPE细胞的间充质上皮转换(Met),我们培养了消化不良的猪RPE(PRPE)细胞并在四种条件下比较了它们的行为:1)在细胞培养皿中,含有FBS的DMEM / F12(CC盘-FBS),2)在培养皿中,含有FBS(培养皿FBS),3)中的DMEM / F12,在培养皿中含有DMEM / F12的细胞培养皿中的DMEM / F12和4) DMEM / F12含有N2和B27(Petri Dish-N2B27)。除了观察细胞形态和行为之外,通过免疫染色,定量实时PCR和Western印迹检查RPE特异性标记以及EMT相关基因和蛋白质。结果表明,消化不良的PRPE细胞在CC盘FBS,培养皿 - FBS和CC盘N2B27组中保持EMT,而当在培养皿-N2B27中培养去分化的PRPE细胞时,诱导鉴定。这种诱导的PRPE细胞显示出多边形形态,随着RPE特异性标记的表达增加和降低的EMT相关标志物。在诱导多能干细胞衍生的RPE细胞中观察到类似的结果。此外,在重新分化的那些去分化的PRPE细胞期间,培养皿-N2B27减少了RhOA的活性并诱导F-Actin重新排列,其促进了用PDZ结合主题(TAZ)和TAZ靶标的转录共激活剂的核排蛋分子锌指E箱结合蛋白(Zeb1),两者都是EMT诱导因子。该研究提供了一种简单且可靠的方法,可以将PRPE细胞的去脱脂表型反转成上皮细胞的上皮化表型,这更适合于在体外研究AMD,并表明可以通过类似的方法诱导其他细胞类型的满足。

著录项

  • 来源
    《Experimental Eye Research》 |2018年第2018期|共13页
  • 作者单位

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

    TUSM Tongji Eye Inst Shanghai Hosp 10 Dept Ophthalmol Shanghai Peoples R China;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 眼科学;
  • 关键词

    RPE; Age-related macular degeneration; Epithelial-mesenchymal transition; Mesenchymal-epithelial transition; TAZ; ZEB1;

    机译:RPE;年龄相关的黄斑变性;上皮 - 间充质转换;间充质 - 上皮过渡;TAZ;Zeb1;

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