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内源性 Oct4 表达调控对脂肪组织基质细胞行为的影响。

Regulation of adipose tissue stromal cells behaviors by endogenic Oct4 expression control.

机构信息

Department of Veterinary Biotechnology, Seoul National University, Seoul, Republic of Korea.

出版信息

PLoS One. 2009 Sep 24;4(9):e7166. doi: 10.1371/journal.pone.0007166.

Abstract

BACKGROUND

To clarify the role of the POU domain transcription factor Oct4 in Adipose Tissue Stromal Cells (ATSCs), we investigated the regulation of Oct4 expression and other embryonic genes in fully differentiated cells, in addition to identifying expression at the gene and protein levels. The ATSCs and several immature cells were routinely expressing Oct4 protein before and after differentiating into specific lineages.

METHODOLOGY/PRINCIPAL FINDINGS AND CONCLUSIONS: Here, we demonstrated the role of Oct4 in ATSCs on cell proliferation and differentiation. Exogenous Oct4 improves adult ATSCs cell proliferation and differentiation potencies through epigenetic reprogramming of stemness genes such as Oct4, Nanog, Sox2, and Rex1. Oct4 directly or indirectly induces ATSCs reprogramming along with the activation of JAK/STAT3 and ERK1/2. Exogenic Oct4 introduced a transdifferentiation priority into the neural lineage than mesodermal lineage. Global gene expression analysis results showed that Oct4 regulated target genes which could be characterized as differentially regulated genes such as pluripotency markers NANOG, SOX2, and KLF4 and markers of undifferentiated stem cells FOXD1, CDC2, and EPHB1. The negatively regulated genes included FAS, TNFR, COL6A1, JAM2, FOXQ1, FOXO1, NESTIN, SMAD3, SLIT3, DKK1, WNT5A, BMP1, and GLIS3 which are implicated in differentiation processes as well as a number of novel genes. Finally we have demonstrated the therapeutic utility of Oct4/ATSCs were introduced into the mouse traumatic brain, engrafted cells was more effectively induces regeneration activity with high therapeutic modality than that of control ATSCs. Engrafted Oct4/ATSCs efficiently migrated and transdifferentiated into action potential carrying, functionally neurons in the hippocampus and promoting the amelioration of lesion cavities.

摘要

背景

为了阐明 POU 结构域转录因子 Oct4 在脂肪组织基质细胞(ATSCs)中的作用,我们研究了完全分化细胞中 Oct4 表达和其他胚胎基因的调节,除了在基因和蛋白水平上进行鉴定。在 ATSCs 以及几种未成熟细胞分化为特定谱系之前和之后,常规表达 Oct4 蛋白。

方法/主要发现和结论:在这里,我们证明了 Oct4 在 ATSCs 细胞增殖和分化中的作用。外源性 Oct4 通过表观遗传重编程干细胞基因(如 Oct4、Nanog、Sox2 和 Rex1)来提高成体 ATSCs 细胞增殖和分化潜能。Oct4 直接或间接诱导 ATSCs 重编程,同时激活 JAK/STAT3 和 ERK1/2。外源性 Oct4 使神经谱系优先于中胚层谱系进行转分化。全基因表达分析结果表明,Oct4 调节的靶基因可被描述为差异调节基因,如多能标记物 NANOG、SOX2 和 KLF4 以及未分化干细胞的标记物 FOXD1、CDC2 和 EPHB1。负调控基因包括 FAS、TNFR、COL6A1、JAM2、FOXQ1、FOXO1、NESTIN、SMAD3、SLIT3、DKK1、WNT5A、BMP1 和 GLIS3,这些基因参与分化过程以及许多新基因。最后,我们证明了 Oct4/ATSCs 被引入小鼠创伤性脑后的治疗效用,与对照 ATSCs 相比,移植细胞更有效地诱导再生活性,具有更高的治疗模式。移植的 Oct4/ATSCs 有效地迁移并转化为具有动作电位的功能性神经元,在海马中促进损伤腔的改善。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/745f/2747014/33c1c9d8d610/pone.0007166.g001.jpg

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