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Using a structural and logics systems approach to infer bHLH–DNA binding specificity determinants

机译:使用结构和逻辑系统方法推断bHLH-DNA结合特异性决定因素

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摘要

Numerous efforts are underway to determine gene regulatory networks that describe physical relationships between transcription factors (TFs) and their target DNA sequences. Members of paralogous TF families typically recognize similar DNA sequences. Knowledge of the molecular determinants of protein–DNA recognition by paralogous TFs is of central importance for understanding how small differences in DNA specificities can dictate target gene selection. Previously, we determined the in vitro DNA binding specificities of 19 Caenorhabditis elegans basic helix-loop-helix (bHLH) dimers using protein binding microarrays. These TFs bind E-box (CANNTG) and E-box-like sequences. Here, we combine these data with logics, bHLH–DNA co-crystal structures and computational modeling to infer which bHLH monomer can interact with which CAN E-box half-site and we identify a critical residue in the protein that dictates this specificity. Validation experiments using mutant bHLH proteins provide support for our inferences. Our study provides insights into the mechanisms of DNA recognition by bHLH dimers as well as a blueprint for system-level studies of the DNA binding determinants of other TF families in different model organisms and humans.
机译:为了确定描述转录因子(TFs)与它们的靶DNA序列之间的物理关系的基因调控网络,正在进行许多努力。旁系TF家族的成员通常识别相似的DNA序列。理解旁源TF对蛋白质-DNA识别的分子决定因素的知识对于理解DNA特异性的微小差异如何决定靶基因选择至关重要。以前,我们使用蛋白质结合微阵列测定了19种秀丽隐杆线虫基本螺旋-环-螺旋(bHLH)二聚体的体外DNA结合特异性。这些TF结合E-box(CANNTG)和E-box-like序列。在这里,我们将这些数据与逻辑,bHLH-DNA共晶体结构和计算模型相结合,以推断哪些bHLH单体可以与哪个CAN E-box半位点相互作用,并在蛋白质中鉴定出决定该特异性的关键残基。使用突变bHLH蛋白的验证实验为我们的推论提供了支持。我们的研究为bHLH二聚体识别DNA的机制提供了见识,并为不同模型生物和人类中其他TF家族的DNA结合决定簇的系统级研究提供了蓝图。

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