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首页> 外文期刊>Journal of Molecular Biology >Structural requirements for cooperative binding of HMG1 to DNA minicircles.
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Structural requirements for cooperative binding of HMG1 to DNA minicircles.

机译:HMG1与DNA小环的协同结合的结构要求。

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摘要

DNA minicircles, where the length of DNA is below the persistence length, are highly effective, preferred, ligands for HMG-box proteins. The proteins bind to them "structure-specifically" with affinities in the nanomolar range, presumably to an exposed widened minor groove. To understand better the basis of this preference, we have studied the binding of HMG1 (which has two tandem HMG boxes linked by a basic extension to a long acidic tail) and Drosophila HMG-D (one HMG box linked by a basic region to a short and less acidic tail), and their HMG-box domains, to 88 bp and 75 bp DNA minicircles. In some cases we see cooperative binding of two molecules to the circles. The requirements for strong cooperativity are two HMG boxes and the basic extension; the latter also appears to stabilize and constrain the complex, preventing binding of further protein molecules. HMG-D, with a single HMG box, does not bind cooperatively. In the case of HMG1, the acidic tail is not required for cooperativity and does not affect binding significantly, in contrast to a much greater effect with linear DNA, or even four-way junctions (another distorted DNA substrate). Such effects could be relevant in the hierarchy of binding of HMG-box proteins to DNA distortions in vivo, where both single-box and two-box proteins might co-exist, with or without basic extensions and acidic tails.
机译:DNA长度小于持久性长度的DNA小圆环是HMG-box蛋白的高效,优选配体。蛋白质以纳摩尔范围内的亲和力“结构特异性”结合到蛋白质上,大概与暴露的加宽小沟相连。为了更好地理解这种偏好的基础,我们研究了HMG1(具有两个串联HMG盒,通过基本延伸与长酸性尾巴相连)和果蝇HMG-D(一个HMG盒,通过基本区域与AMG相连)的结合。短而酸性较低的尾巴)及其HMG-box结构域,分别为88 bp和75 bp DNA小环。在某些情况下,我们看到两个分子协同结合到圆上。强大的协作性要求是两个HMG盒子和基本扩展;后者也似乎稳定和约束了复合物,阻止了其他蛋白质分子的结合。具有单个HMG框的HMG-D无法协同绑定。在HMG1的情况下,协同作用不需要酸性尾部,并且不会显着影响结合,这与线性DNA甚至四向连接(另一种扭曲的DNA底物)产生的影响大得多。这种作用可能与体内HMG盒蛋白与DNA变形的结合层次有关,在这种情况下,单盒蛋白和两盒蛋白都可能共存,带有或不带有碱性延伸和酸性尾巴。

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