Literature DB >> 21910138

MCCE analysis of the pKas of introduced buried acids and bases in staphylococcal nuclease.

M R Gunner1, Xuyu Zhu, Max C Klein.   

Abstract

The pK(a)s of 96 acids and bases introduced into buried sites in the staphylococcal nuclease protein (SNase) were calculated using the multiconformation continuum electrostatics (MCCE) program and the results compared with experimental values. The pK(a)s are obtained by Monte Carlo sampling of coupled side chain protonation and position as a function of pH. The dependence of the results on the protein dielectric constant (ε(prot)) in the continuum electrostatics analysis and on the Lennard-Jones non-electrostatics parameters was evaluated. The pK(a)s of the introduced residues have a clear dependence on ε(prot,) whereas native ionizable residues do not. The native residues have electrostatic interactions with other residues in the protein favoring ionization, which are larger than the desolvation penalty favoring the neutral state. Increasing ε(prot) scales both terms, which for these residues leads to small changes in pK(a). The introduced residues have a larger desolvation penalty and negligible interactions with residues in the protein. For these residues, changing ε(prot) has a large influence on the calculated pK(a). An ε(prot) of 8-10 and a Lennard-Jones scaling of 0.25 is best here. The X-ray crystal structures of the mutated proteins are found to provide somewhat better results than calculations carried out on mutations made in silico. Initial relaxation of the in silico mutations by Gromacs and extensive side chain rotamer sampling within MCCE can significantly improve the match with experiment.
Copyright © 2011 Wiley-Liss, Inc.

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Year:  2011        PMID: 21910138     DOI: 10.1002/prot.23124

Source DB:  PubMed          Journal:  Proteins        ISSN: 0887-3585


  22 in total

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Review 8.  Continuum Electrostatics Approaches to Calculating pKas and Ems in Proteins.

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