首页> 外文期刊>The Journal of biological chemistry >Generation of Induced Pluripotent Stem Cells from Human Renal Proximal Tubular Cells with Only Two Transcription Factors, Oct4 and Sox2
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Generation of Induced Pluripotent Stem Cells from Human Renal Proximal Tubular Cells with Only Two Transcription Factors, Oct4 and Sox2

机译:从人肾近端管状细胞产生诱导多能干细胞,只有两个转录因子,OCT4和SOX2

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The tubular epithelium of the kidney is susceptible to injury from a number of different causes, including inflammatory and immune disorders, oxidative stress, and nephrotoxins, among others. Primary renal epithelial cells remain one of the few tools for studying the biochemical and physiological characteristics of the renal tubular system. Nevertheless, differentiated primary cells are not suitable for recapitulation of disease properties that might arise during embryonic kidney formation and further maturation. Thus, cellular systems resembling kidney characteristics are in urgent need to model disease as well as to establish reliable drug-testing platforms. Induced pluripotent stem cells (iPSCs) bear the capacity to differentiate into every cell lineage comprising the adult organism. Thus, iPSCs bring the possibility for recapitulating embryonic development by directed differentiation into specific lineages. iPSC differentiation ultimately allows for both disease modeling in vitro and the production of cellular products with potential for regenerative medicine. Here, we describe the rapid, reproducible, and highly efficient generation of iPSCs derived from endogenous kidney tubular renal epithelial cells with only two transcriptional factors, OCT4 and SOX2. Kidney-derived iPSCs may provide a reliable cellular platform for the development of kidney differentiation protocols allowing drug discovery studies and the study of kidney pathology.
机译:肾脏的管状上皮易受许多不同原因的损伤,包括炎症和免疫紊乱,氧化应激和肾毒素等。原代肾上皮细胞仍然是研究肾小管系统的生化和生理特性的少数工具之一。然而,分化的原代细胞不适合于胚胎肾形成期间可能出现的疾病性质和进一步成熟的疾病性质。因此,与肾特征类似的细胞系统迫切需要模拟疾病,并建立可靠的药物测试平台。诱导多能干细胞(IPSCS)承担分化到包含成人生物的每个细胞谱系的能力。因此,IPSCS通过指向特定谱系将胚胎发育重新构成胚胎发育。 IPSC分化最终允许体外疾病建模和生产细胞产品,其具有再生药物的潜力。在这里,我们描述了源自内源性肾小管肾上皮细胞的快速,可重复和高效的IPSC,只有两个转录因子,OCT4和SOX2。肾脏衍生的IPSC可以为肾脏分化方案的发展提供可靠的细胞平台,允许药物发现研究和肾脏病理学研究。

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