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ReadOut: structure-based calculation of direct and indirect readout energies and specificities for protein–DNA recognition

机译:读出:基于结构的直接和间接读出能量以及蛋白质-DNA识别特异性的计算

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摘要

Protein–DNA interactions play a central role in regulatory processes at the genetic level. DNA-binding proteins recognize their targets by direct base–amino acid interactions and indirect conformational energy contribution from DNA deformations and elasticity. Knowledge-based approach based on the statistical analysis of protein–DNA complex structures has been successfully used to calculate interaction energies and specificities of direct and indirect readouts in protein–DNA recognition. Here, we have implemented the method as a webserver, which calculates direct and indirect readout energies and Z-scores, as a measure of specificity, using atomic coordinates of protein–DNA complexes. This server is freely available at . The only input to this webserver is the Protein Data Bank (PDB) style coordinate data of atoms or the PDB code itself. The server returns total energy Z-scores, which estimate the degree of sequence specificity of the protein–DNA complex. This webserver is expected to be useful for estimating interaction energy and DNA conformation energy, and relative contributions to the specificity from direct and indirect readout. It may also be useful for checking the quality of protein–DNA complex structures, and for engineering proteins and target DNAs.
机译:蛋白质与DNA的相互作用在遗传水平的调节过程中起着核心作用。 DNA结合蛋白通过直接的碱基氨基酸相互作用以及DNA变形和弹性产生的间接构象能量来识别其靶标。基于蛋白质-DNA复杂结构的统计分析的基于知识的方法已成功用于计算蛋白质-DNA识别中相互作用能和直接和间接读数的特异性。在这里,我们将这种方法实现为网络服务器,该网络服务器使用蛋白质-DNA复合物的原子坐标来计算直接和间接读出的能量和Z分数,以此来衡量特异性。该服务器可从以下位置免费获得。该Web服务器的唯一输入是原子的蛋白质数据库(PDB)样式坐标数据或PDB代码本身。服务器返回总能量Z分数,该分数可估计蛋白质-DNA复合物的序列特异性程度。该网络服务器有望用于估计相互作用能和DNA构象能,以及直接和间接读出对特异性的相对贡献。它对于检查蛋白质-DNA复杂结构的质量以及工程化蛋白质和目标DNA可能也很有用。

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