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Binding of Transcription Factor GabR to DNA Requires Recognition of DNA Shape at a Location Distinct from its Cognate Binding Site

机译:转录因子GabR与DNA的结合需要识别与其同源结合位点不同的DNA形状。

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摘要

Mechanisms for transcription factor recognition of specific DNA base sequences are well characterized and recent studies demonstrate that the shape of these cognate binding sites is also important. Here, we uncover a new mechanism where the transcription factor GabR simultaneously recognizes two cognate binding sites and the shape of a 29 bp DNA sequence that bridges these sites. Small-angle X-ray scattering and multi-angle laser light scattering are consistent with a model where the DNA undergoes a conformational change to bend around GabR during binding. In silico predictions suggest that the bridging DNA sequence is likely to be bendable in one direction and kinetic analysis of mutant DNA sequences with biolayer interferometry, allowed the independent quantification of the relative contribution of DNA base and shape recognition in the GabR–DNA interaction. These indicate that the two cognate binding sites as well as the bendability of the DNA sequence in between these sites are required to form a stable complex. The mechanism of GabR–DNA interaction provides an example where the correct shape of DNA, at a clearly distinct location from the cognate binding site, is required for transcription factor binding and has implications for bioinformatics searches for novel binding sites.
机译:转录因子识别特定DNA碱基序列的机制已得到充分表征,最近的研究表明这些同源结合位点的形状也很重要。在这里,我们发现了一种新的机制,其中转录因子GabR同时识别两个同源结合位点和桥接这些位点的29 bp DNA序列的形状。小角度X射线散射和多角度激光散射与在结合过程中DNA经历构象变化以围绕GabR弯曲的模型一致。在计算机上的预测表明,桥接的DNA序列可能在一个方向上是可弯曲的,并且利用生物层干涉术对突变的DNA序列进行动力学分析,可以独立定量DNA碱基的相对贡献和形状识别在GabR-DNA相互作用中的作用。这些表明需要两个同源结合位点以及这些位点之间的DNA序列的可弯曲性以形成稳定的复合物。 GabR–DNA相互作用的机制提供了一个示例,其中转录因子结合需要与同源结合位点明显不同的正确形状的DNA,这对于寻找新的结合位点的生物信息学具有重要意义。

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