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Linkage of pluripotent stem cell-associated transcripts to regulatory gene networks.

机译:多能干细胞相关转录本与调控基因网络的联系。

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摘要

Knowledge of the transcriptional circuitry responsible for pluripotentiality and self-renewal in embryonic stem cells is tantamount to understanding early mammalian development and a prerequisite to determining their therapeutic potential. Various techniques have employed genomics to identify transcripts that were abundant in stem cells, in an attempt to define the molecular basis of 'stemness'. In this study, we have extended traditional genomic analyses to identify cis-elements that might be implicated in the control of embryonic stem cell-restricted gene promoters. The strategy relied on the generation of a problem-specific list from serial analysis of gene expression profiles and subsequent promoter analyses to identify frameworks of multiple cis-elements conserved in space and orientation among genes from the problem-specific list. Subsequent experimental data suggest that 2 novel transcription factors, B-Myb and Maz, predicted from these models, are implicated either in the maintenance of the undifferentiated stem cell state or in early steps of differentiation.
机译:对负责胚胎干细胞多能性和自我更新的转录途径的了解,无异于理解哺乳动物的早期发育以及确定其治疗潜力的前提。为了定义“干性”的分子基础,各种技术已采用基因组学来鉴定在干细胞中丰富的转录本。在这项研究中,我们扩展了传统的基因组分析,以识别可能与控制胚胎干细胞限制性基因启动子有关的顺式元件。该策略依靠从基因表达谱的系列分析和随后的启动子分析中生成问题特定列表,以从问题特定列表中识别基因之间在空间和方向上保守的多个顺式元件的框架。随后的实验数据表明,根据这些模型预测的2种新的转录因子B-Myb和Maz与未分化干细胞状态的维持或分化的早期阶段有关。

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