Department of Biology, California State University Northridge, 18111 Nordhoff St. Northridge, CA 91330, USA.
Nucleic Acids Res. 2011 Aug;39(15):6813-24. doi: 10.1093/nar/gkr369. Epub 2011 May 17.
We show that the cAMP receptor protein (Crp) binds to DNA as several different conformers. This situation has precluded discovering a high correlation between any sequence property and binding affinity for proteins that bend DNA. Experimentally quantified affinities of Synechocystis sp. PCC 6803 cAMP receptor protein (SyCrp1), the Escherichia coli Crp (EcCrp, also CAP) and DNA were analyzed to mathematically describe, and make human-readable, the relationship of DNA sequence and binding affinity in a given system. Here, sequence logos and weight matrices were built to model SyCrp1 binding sequences. Comparing the weight matrix model to binding affinity revealed several distinct binding conformations. These Crp/DNA conformations were asymmetrical (non-palindromic).
我们表明,cAMP 受体蛋白 (Crp) 以几种不同的构象结合 DNA。这种情况使得很难发现任何序列特性与弯曲 DNA 的蛋白质之间的结合亲和力之间存在高度相关性。对 Synechocystis sp. PCC 6803 cAMP 受体蛋白 (SyCrp1)、大肠杆菌 Crp(EcCrp,也称为 CAP)和 DNA 的实验量化亲和力进行了分析,以数学方式描述并使给定系统中的 DNA 序列和结合亲和力具有可读性。在这里,构建了序列标志和权重矩阵来模拟 SyCrp1 结合序列。将权重矩阵模型与结合亲和力进行比较,揭示了几种不同的结合构象。这些 Crp/DNA 构象是不对称的(非回文)。
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