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miR-290-295 簇通过调节小鼠胚胎干细胞的细胞周期分布来促进多能性维持。

The miR-290-295 cluster promotes pluripotency maintenance by regulating cell cycle phase distribution in mouse embryonic stem cells.

机构信息

Agricultural Biotechnology Center, H-2100, Szent-Györgyi A, Str. 4, Gödöllő, Hungary.

出版信息

Differentiation. 2011 Jan;81(1):11-24. doi: 10.1016/j.diff.2010.08.002. Epub 2010 Sep 22.

Abstract

The mmu-miR-290-295 cluster codes for a family of microRNAs (miRNAs) that are expressed de novo during early embryogenesis and are specific for mouse embryonic stem cells (ESC) and embryonic carcinoma cells (ECC). Detailed sequence analysis and alignment studies of miR-290-295 precursors demonstrated that the cluster has evolved by repeated duplication events of the ancient miR-290 precursor. We show that under serum starvation, overexpression of miR-290-295 miRNAs withhold ES cells from early differentiation, ensures their high proliferation rate and capacity for forming alkaline phosphate positive colonies. Transcriptome analysis revealed that differentiation related marker genes are underexpressed upon high miR-290-295 level. Importantly, miR-290-295 overexpression prevents ES cells from accumulation in G1 phase at low serum level, and seems to regulate cell cycle in different phases. Our data underline that miR-290-295 miRNAs contribute to the natural absence of G1 checkpoint in embryonic stem cells. We define the cell cycle regulators Wee1 and Fbxl5 as potential direct targets of miR-290-295 miRNAs in vitro. Our results suggest that miR-290-295 miRNAs exhibit their effect predominantly through the regulation of cell cycle phase distribution.

摘要

mmu-miR-290-295 簇编码了一组 miRNA,它们在早期胚胎发生过程中从头表达,特异性表达于小鼠胚胎干细胞(ESC)和胚胎癌细胞(ECC)。miR-290-295 前体的详细序列分析和比对研究表明,该簇通过古老的 miR-290 前体的重复复制事件进化而来。我们表明,在血清饥饿下,miR-290-295 miRNA 的过表达阻止 ES 细胞早期分化,确保其高增殖率和形成碱性磷酸酶阳性集落的能力。转录组分析显示,高 miR-290-295 水平下分化相关标记基因表达下调。重要的是,miR-290-295 的过表达可防止 ES 细胞在低血清水平时在 G1 期积累,并似乎在不同阶段调节细胞周期。我们的数据表明,miR-290-295 miRNA 有助于胚胎干细胞中天然不存在 G1 检验点。我们确定细胞周期调节剂 Wee1 和 Fbxl5 为 miR-290-295 miRNA 在体外的潜在直接靶标。我们的结果表明,miR-290-295 miRNA 主要通过调节细胞周期相分布来发挥作用。

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