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miR-191 modulates B-cell development and targets transcription factors E2A, Foxp1, and Egr1

机译:mir - 191调节b细胞发育和目标转录因子ea2、Foxp1 Egr1

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摘要

The interdependence of posttranscriptional gene regulation via miRNA and transcriptional regulatory networks in lymphocyte development is poorly understood. Here, we identified miR-191 as direct upstream modulator of a transcriptional module comprising the transcription factors Foxp1, E2A, and Egr1. Deletion as well as ectopic expression of miR-191 resulted in developmental arrest in B lineage cells, indicating that fine tuning of the combined expression levels of Foxp1, E2A, and Egr1, which in turn control somatic recombination and cytokine-driven expansion, constitutes a prerequisite for efficient B-cell development. In conclusion, we propose that miR-191 acts as a rheostat in B-cell development by fine tuning a key transcriptional program.
机译:转录后的基因的相互依存监管通过microrna和转录监管网络在淋巴细胞的发展知之甚少。直接上游转录的调制器模块包括转录因子Foxp1、ea2 Egr1。mir - 191的表达导致发育在B细胞谱系被捕,这表明好优化的组合表达水平Foxp1、ea2 Egr1,进而控制体细胞重组和cytokine-driven扩张,构成一个先决条件高效的b细胞的发展。建议mir - 191作为一个变阻器在b细胞开发通过微调关键转录程序。

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