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DNA-binding specificities of human transcription factors

机译:人类转录因子的DNA结合特异性

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Although the proteins that read the gene regulatory code, transcription factors (TFs), have been largely identified, it is not well known which sequences TFs can recognize. We have analyzed the sequence-specific binding of human TFs using high-throughput SELEX and ChIP sequencing. A total of 830 binding profiles were obtained, describing 239 distinctly different binding specificities. The models represent the majority of human TFs, approximately doubling the coverage compared to existing systematic studies. Our results reveal additional specificity determinants for a large number of factors for which a partial specificity was known, including a commonly observed A- or T-rich stretch that flanks the core motifs. Global analysis of the data revealed that homodimer orientation and spacing preferences, and base-stacking interactions, have a larger role in TF-DNA binding than previously appreciated. We further describe a binding model incorporating these features that is required to understand binding of TFs to DNA.
机译:尽管已经大量鉴定了读取基因调控密码的蛋白质,即转录因子(TFs),但尚不清楚TFs可以识别哪些序列。我们已经分析了使用高通量SELEX和ChIP测序的人TF的序列特异性结合。总共获得了830个结合图谱,描述了239个明显不同的结合特异性。这些模型代表了大多数人类TF,与现有的系统研究相比,覆盖率大约翻了一番。我们的结果揭示了许多因素的其他特异性决定因素,这些因素的部分特异性已知,包括通常观察到侧翼于核心基序的富含A或T的延伸序列。数据的整体分析表明,同二聚体的取向和间隔偏好以及碱基堆积相互作用在TF-DNA结合中的作用比以前认识的要大。我们进一步描述结合模型,这些模型是理解TF与DNA结合所必需的。

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