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Discovery optimization and validation of an optimal DNA-binding sequence for the Six1 homeodomain transcription factor

机译:发现优化和验证Six1同源域转录因子的最佳DNA结合序列。

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摘要

The Six1 transcription factor is a homeodomain protein involved in controlling gene expression during embryonic development. Six1 establishes gene expression profiles that enable skeletal myogenesis and nephrogenesis, among others. While several homeodomain factors have been extensively characterized with regards to their DNA-binding properties, relatively little is known of the properties of Six1. We have used the genomic binding profile of Six1 during the myogenic differentiation of myoblasts to obtain a better understanding of its preferences for recognizing certain DNA sequences. DNA sequence analyses on our genomic binding dataset, combined with biochemical characterization using binding assays, reveal that Six1 has a much broader DNA-binding sequence spectrum than had been previously determined. Moreover, using a position weight matrix optimization algorithm, we generated a highly sensitive and specific matrix that can be used to predict novel Six1-binding sites with highest accuracy. Furthermore, our results support the idea of a mode of DNA recognition by this factor where Six1 itself is sufficient for sequence discrimination, and where Six1 domains outside of its homeodomain contribute to binding site selection. Together, our results provide new light on the properties of this important transcription factor, and will enable more accurate modeling of Six1 function in bioinformatic studies.
机译:Six1转录因子是一个同源结构域蛋白,参与胚胎发育过程中的基因表达控制。 Six1建立了基因表达谱,使骨骼肌发生和肾发生等成为可能。尽管已经对几种同源结构域因子的DNA结合特性进行了广泛表征,但对Six1的特性知之甚少。我们在成肌细胞的成肌分化过程中使用了Six1的基因组结合图谱,以更好地了解其识别某些DNA序列的偏好。在我们的基因组结合数据集上进行的DNA序列分析,结合使用结合测定法进行的生化表征,揭示出Six1具有比以前确定的更广泛的DNA结合序列光谱。此外,使用位置权重矩阵优化算法,我们生成了高度敏感且特定的矩阵,可用于预测最高精度的新颖Six1结合位点。此外,我们的研究结果支持通过该因子进行DNA识别的想法,其中Six1本身足以进行序列区分,而其同源结构域之外的Six1结构域则有助于结合位点的选择。总之,我们的结果为这一重要转录因子的特性提供了新的思路,并将使在生物信息学研究中对Six1功能的建模更为准确。

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