Protein electrostatics and pKa blind predictions; contribution from empirical predictions of internal ionizable residues

Mats H. M. Olsson

doi:10.1002/prot.23113

Protein electrostatics and pKa blind predictions; contribution from empirical predictions of internal ionizable residues

Mats H. M. Olsson

Department of Chemistry

30 Citations (Scopus)

Abstract

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.

Original language	English
Journal	Proteins: Structure, Function, and Bioinformatics
Volume	79
Issue number	12
Pages (from-to)	3333-3345
Number of pages	13
ISSN	0887-3585
DOIs	https://doi.org/10.1002/prot.23113
Publication status	Published - Dec 2011

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title = "Protein electrostatics and pKa blind predictions; contribution from empirical predictions of internal ionizable residues",

abstract = "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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AU - Olsson, Mats H. M.

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AB - 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.

U2 - 10.1002/prot.23113

DO - 10.1002/prot.23113

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JO - Proteins: Structure, Function, and Bioinformatics

JF - Proteins: Structure, Function, and Bioinformatics

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Protein electrostatics and pKa blind predictions; contribution from empirical predictions of internal ionizable residues

Abstract

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