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(66e) Regulatory Role of Tandem Repeats Containing Transcription Factor Binding Sites

机译:(66E)串联重复含有转录因子结合位点的调节作用

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Tandem repeats of DNA are widely prevalent in higher eukaryotic genomes. Because their growth and decay can occur after only a few generations, the lengths of these tracts are often hypervariable and vary between individuals. Here we explore the regulatory impact that tandem repeats of DNA that contain transcription factor (TF) binding sites can have on gene expression, using a synthetic biology approach in budding yeast. Not surprisingly, we find that the addition of arrays of repeated binding sites for a transcriptionai activator competitively inhibit the normal TF-promoter interactions and reduce gene expression. More surprisingly, the repeat sites convert the linear dose-response of the promoter with respect to the TF into a more ultrasensitive response. This can be explained by a model whereby the repeat sites have 10-100 fold higher affinity to the TF compared with the promoter. We discuss the origins and implications of this difference and demonstrate how the changes in the repeat number of off-target binding sites can qualitatively affect gene regulation.
机译:DNA的串联重复在高等真核基因组中广泛普遍。因为只有几代人的成长和衰减可能发生,所以这些尸体的长度往往是多变质和各个人之间的变化。在这里,我们探讨了含有转录因子(TF)结合位点的DNA的串联重复的调节效果,可以在萌芽酵母中使用合成生物学方法对基因表达进行基因表达。毫不奇怪,我们发现,对转移激活剂的重复结合位点的阵列竞争性地抑制正常的TF启动子相互作用并降低基因表达。更令人惊讶的是,重复位点将启动子的线性剂量反应相对于TF转换为更超细的反应。这可以通过模型解释,由此与启动子相比,重复位点对TF具有10-100倍的亲和力。我们讨论这种差异的起源和含义,并证明了偏离靶标结合位点的重复数量的变化可以定性地影响基因调控。

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