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全面的微小RNA分析揭示了一种独特的人类胚胎干细胞特征,该特征由单个种子序列主导。

Comprehensive microRNA profiling reveals a unique human embryonic stem cell signature dominated by a single seed sequence.

作者信息

Laurent Louise C, Chen Jing, Ulitsky Igor, Mueller Franz-Josef, Lu Christina, Shamir Ron, Fan Jian-Bing, Loring Jeanne F

机构信息

The Scripps Research Institute, 10550 North Torrey Pines Road, La Jolla, California 92037, USA.

出版信息

Stem Cells. 2008 Jun;26(6):1506-16. doi: 10.1634/stemcells.2007-1081. Epub 2008 Apr 10.

DOI:10.1634/stemcells.2007-1081
PMID:18403753
Abstract

Embryonic stem cells are unique among cultured cells in their ability to self-renew and differentiate into a wide diversity of cell types, suggesting that a specific molecular control network underlies these features. Human embryonic stem cells (hESCs) are known to have distinct mRNA expression, global DNA methylation, and chromatin profiles, but the involvement of high-level regulators, such as microRNAs (miRNA), in the hESC-specific molecular network is poorly understood. We report that global miRNA expression profiling of hESCs and a variety of stem cell and differentiated cell types using a novel microarray platform revealed a unique set of miRNAs differentially regulated in hESCs, including numerous miRNAs not previously linked to hESCs. These hESC-associated miRNAs were more likely to be located in large genomic clusters, and less likely to be located in introns of coding genes. hESCs had higher expression of oncogenic miRNAs and lower expression of tumor suppressor miRNAs than the other cell types. Many miRNAs upregulated in hESCs share a common consensus seed sequence, suggesting that there is cooperative regulation of a critical set of target miRNAs. We propose that miRNAs are coordinately controlled in hESCs, and are key regulators of pluripotence and differentiation. Disclosure of potential conflicts of interest is found at the end of this article.

摘要

胚胎干细胞在培养细胞中独具特色,具有自我更新能力,并能分化为多种不同类型的细胞,这表明特定的分子控制网络是这些特性的基础。已知人类胚胎干细胞(hESCs)具有独特的mRNA表达、全基因组DNA甲基化和染色质谱,但对于诸如微小RNA(miRNA)等高级调节因子在hESC特异性分子网络中的作用,人们了解甚少。我们报告称,利用一种新型微阵列平台对hESCs以及多种干细胞和分化细胞类型进行全基因组miRNA表达谱分析,发现了一组在hESCs中差异调节的独特miRNAs,其中包括许多以前未与hESCs相关联的miRNAs。这些与hESCs相关的miRNAs更有可能位于大型基因组簇中,而不太可能位于编码基因的内含子中。与其他细胞类型相比,hESCs中致癌miRNAs的表达较高,而肿瘤抑制miRNAs的表达较低。许多在hESCs中上调的miRNAs共享一个共同的共有种子序列,这表明对一组关键靶miRNAs存在协同调节。我们提出,miRNAs在hESCs中受到协同控制,并且是多能性和分化的关键调节因子。潜在利益冲突的披露见本文末尾。

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