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Predicting PDZ domain-peptide interactions from primary sequences.

机译:从一级序列预测PDZ结构域-肽的相互作用。

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摘要

PDZ domains constitute one of the largest families of interaction domains and function by binding the C termini of their target proteins. Using Bayesian estimation, we constructed a three-dimensional extension of a position-specific scoring matrix that predicts to which peptides a PDZ domain will bind, given the primary sequences of the PDZ domain and the peptides. The model, which was trained using interaction data from 82 PDZ domains and 93 peptides encoded in the mouse genome, successfully predicts interactions involving other mouse PDZ domains, as well as PDZ domains from Drosophila melanogaster and, to a lesser extent, PDZ domains from Caenorhabditis elegans. The model also predicts the differential effects of point mutations in peptide ligands on their PDZ domain-binding affinities. Overall, we show that our approach captures, in a single model, the binding selectivity of the PDZ domain family.
机译:PDZ结构域构成相互作用结构域的最大家族之一,并通过结合其靶蛋白的C末端发挥功能。使用贝叶斯估计,我们构建了位置特异性得分矩阵的三维扩展,该矩阵预测了给定PDZ域和肽段的原始序列的PDZ域将与哪些肽结合。使用来自小鼠基因组中82个PDZ域和93个肽段的相互作用数据对模型进行了训练,该模型成功预测了涉及其他小鼠PDZ域以及黑腹果蝇(Drosophila melanogaster)的PDZ域以及在较小程度上来自秀丽隐杆线虫(Caenorhabditis)的PDZ域的相互作用线虫。该模型还预测了肽配体中的点突变对其PDZ域结合亲和力的不同影响。总体而言,我们表明,我们的方法在单个模型中捕获了PDZ域家族的结合选择性。

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