In this study, we validate and probe the description of electrostatic interactions within proteins by predicting and comparing pK(a) values of ionizable groups in a series of mutated staphylococcal nuclease variants with experiments. This set of pK(a) values is found to be the most challenging pK(a) data to date, because ionizable residues have been introduced in hydrophobic patches in the protein interior and are therefore significantly shifted from their reference solvated values. We find that using PROPKA2 (Li et al., Proteins 2005;61:704-721) results in an rmsd value close to 2 for true blind predictions (1.6 if we reassign the tightly coupled Asp19/21 pair) and close to 1 for postpredictions with the newly developed PROPKA3 (Olsson et al., J. Chem. Theor. Comp. 2011;7:525-537). We also use the performance of the Null-model, predictions made with the reference value only, to provide a better description of the expected errors in pK(a) predictions and to compare submissions made using different subsets of the pK(a) data more consistently.
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机译:在这项研究中,我们通过预测和比较一系列突变葡萄球菌核酸酶变异体中可电离基团的pK(a)值,通过实验验证并探测了蛋白质内静电相互作用的描述。这套pK(a)值被认为是迄今为止最具挑战性的pK(a)数据,因为可电离的残基已被引入蛋白质内部的疏水性斑块中,因此与参考溶剂化值有明显的偏离。我们发现使用PROPKA2(Li et al。,Proteins 2005; 61:704-721)得出的真均方根值的均方根值接近2(如果我们重新分配紧密耦合的Asp19 / 21对,则均方根值接近1.6)新开发的PROPKA3进行事后预测(Olsson等,J。Chem。Theor。Comp。2011; 7:525-537)。我们还使用Null模型的性能(仅使用参考值进行预测)来更好地描述pK(a)预测中的预期误差,并比较使用pK(a)数据的不同子集提交的提交内容。始终如一。
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