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Encounters across networks: Windows into principles of genomic regulation

机译:遍历网络:窗户进入基因组规则的原则

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Gene regulatory networks account for the ability of the genome to program development in complex multi cellular organisms. Such networks are based on principles of gene regulation by combinations of transcription factors that bind to specific cis-regulatory DNA sites to activate transcription. These cis-regulatory regions mediate logic processing at each network node, enabling progressive increases in organismal complexity with development. Gene regulatory network explanations of development have been shown to account for patterning and cell type diversification in fly and sea urchin embryonic systems, where networks are characterized by fast coupling between transcriptional inputs and changes in target gene transcription rates, and crucial cis-regulatory elements are concentrated relatively close to the protein coding sequences of the target genes, thus facilitating their identification. Stem cell-based development in post-embryonic mammalian systems also depends on gene networks, but differs from the fly and sea urchin systems. First, the number of regulatory elements per gene and the distances between regulatory elements and the genes they control are considerably larger, forcing searches via genome-wide transcription factor binding surveys rather than functional assays. Second, the intrinsic timing of network state transitions can be slowed considerably by the need to undo stem-cell chromatin configurations, which presumably add stability to stem-cell states but retard responses to transcription factor changes during differentiation. The dispersed, partially redundant cis-regulatory systems controlling gene expression and the slow state transition kinetics in these systems already reveal new insights and opportunities to extend understanding of the repertoire of gene networks and regulatory system logic.
机译:基因监管网络占基因组在复杂多细胞生物中进行编程开发的能力。这些网络基于通过结合特异性顺式调节DNA位点的转录因子组合来激活转录的转录因子的基因调节原理。这些顺式调节区域在每个网络节点调解逻辑处理,从而实现了发展的有机体复杂性的逐步增加。已经证明了基因监管网络的开发解释是在飞行和海胆胚胎系统中进行图案化和细胞类型多样化,其中网络的特征在于转录输入与靶基因转录率的变化之间的快速耦合,以及关键的顺式调节元件浓缩相对接近靶基因的蛋白质编码序列,从而促进其鉴定。胚胎后哺乳动物系统的干细胞的发育也取决于基因网络,但与飞行和海胆系统不同。首先,每种基因的调节元件数量和调节元件之间的距离和它们控制的基因相当大,通过基因组转录因子结合调查而非功能测定,强制搜索。其次,通过撤消茎细胞染色质构型的需要,可以大大减慢网络状态转变的内在时序,这可能会增加茎细胞状态的稳定性,而是在分化期间延迟对转录因子变化的反应。控制基因表达的分散的部分冗余的顺式调节系统和这些系统中的缓慢状态转换动力学已经揭示了延长了解基因网络曲目和监管系统逻辑的理解的新见解和机会。

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