Autofix for backward-fit sidechains: using MolProbity and real-space refinement to put misfits in their place

Misfit sidechains in protein crystal structures are a stumbling block in using those structures to direct further scientific inference. Problems due to surface disorder and poor electron density are very difficult to address, but a large class of systematic errors are quite common even in well-order...

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Autores principales: Headd, Jeffrey J., Immormino, Robert M., Keedy, Daniel A., Emsley, Paul, Richardson, David C., Richardson, Jane S.
Formato: Texto
Lenguaje:English
Publicado: Springer Netherlands 2008
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2704614/
https://www.ncbi.nlm.nih.gov/pubmed/19002604
http://dx.doi.org/10.1007/s10969-008-9045-8
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author Headd, Jeffrey J.
Immormino, Robert M.
Keedy, Daniel A.
Emsley, Paul
Richardson, David C.
Richardson, Jane S.
author_facet Headd, Jeffrey J.
Immormino, Robert M.
Keedy, Daniel A.
Emsley, Paul
Richardson, David C.
Richardson, Jane S.
author_sort Headd, Jeffrey J.
collection PubMed
description Misfit sidechains in protein crystal structures are a stumbling block in using those structures to direct further scientific inference. Problems due to surface disorder and poor electron density are very difficult to address, but a large class of systematic errors are quite common even in well-ordered regions, resulting in sidechains fit backwards into local density in predictable ways. The MolProbity web site is effective at diagnosing such errors, and can perform reliable automated correction of a few special cases such as 180° flips of Asn or Gln sidechain amides, using all-atom contacts and H-bond networks. However, most at-risk residues involve tetrahedral geometry, and their valid correction requires rigorous evaluation of sidechain movement and sometimes backbone shift. The current work extends the benefits of robust automated correction to more sidechain types. The Autofix method identifies candidate systematic, flipped-over errors in Leu, Thr, Val, and Arg using MolProbity quality statistics, proposes a corrected position using real-space refinement with rotamer selection in Coot, and accepts or rejects the correction based on improvement in MolProbity criteria and on χ angle change. Criteria are chosen conservatively, after examining many individual results, to ensure valid correction. To test this method, Autofix was run and analyzed for 945 representative PDB files and on the 50S ribosomal subunit of file 1YHQ. Over 40% of Leu, Val, and Thr outliers and 15% of Arg outliers were successfully corrected, resulting in a total of 3,679 corrected sidechains, or 4 per structure on average. Summary Sentences: A common class of misfit sidechains in protein crystal structures is due to systematic errors that place the sidechain backwards into the local electron density. A fully automated method called “Autofix” identifies such errors for Leu, Val, Thr, and Arg and corrects over one third of them, using MolProbity validation criteria and Coot real-space refinement of rotamers. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1007/s10969-008-9045-8) contains supplementary material, which is available to authorized users.
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spelling pubmed-27046142009-07-01 Autofix for backward-fit sidechains: using MolProbity and real-space refinement to put misfits in their place Headd, Jeffrey J. Immormino, Robert M. Keedy, Daniel A. Emsley, Paul Richardson, David C. Richardson, Jane S. J Struct Funct Genomics Article Misfit sidechains in protein crystal structures are a stumbling block in using those structures to direct further scientific inference. Problems due to surface disorder and poor electron density are very difficult to address, but a large class of systematic errors are quite common even in well-ordered regions, resulting in sidechains fit backwards into local density in predictable ways. The MolProbity web site is effective at diagnosing such errors, and can perform reliable automated correction of a few special cases such as 180° flips of Asn or Gln sidechain amides, using all-atom contacts and H-bond networks. However, most at-risk residues involve tetrahedral geometry, and their valid correction requires rigorous evaluation of sidechain movement and sometimes backbone shift. The current work extends the benefits of robust automated correction to more sidechain types. The Autofix method identifies candidate systematic, flipped-over errors in Leu, Thr, Val, and Arg using MolProbity quality statistics, proposes a corrected position using real-space refinement with rotamer selection in Coot, and accepts or rejects the correction based on improvement in MolProbity criteria and on χ angle change. Criteria are chosen conservatively, after examining many individual results, to ensure valid correction. To test this method, Autofix was run and analyzed for 945 representative PDB files and on the 50S ribosomal subunit of file 1YHQ. Over 40% of Leu, Val, and Thr outliers and 15% of Arg outliers were successfully corrected, resulting in a total of 3,679 corrected sidechains, or 4 per structure on average. Summary Sentences: A common class of misfit sidechains in protein crystal structures is due to systematic errors that place the sidechain backwards into the local electron density. A fully automated method called “Autofix” identifies such errors for Leu, Val, Thr, and Arg and corrects over one third of them, using MolProbity validation criteria and Coot real-space refinement of rotamers. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1007/s10969-008-9045-8) contains supplementary material, which is available to authorized users. Springer Netherlands 2008-11-11 2009-03 /pmc/articles/PMC2704614/ /pubmed/19002604 http://dx.doi.org/10.1007/s10969-008-9045-8 Text en © The Author(s) 2008
spellingShingle Article
Headd, Jeffrey J.
Immormino, Robert M.
Keedy, Daniel A.
Emsley, Paul
Richardson, David C.
Richardson, Jane S.
Autofix for backward-fit sidechains: using MolProbity and real-space refinement to put misfits in their place
title Autofix for backward-fit sidechains: using MolProbity and real-space refinement to put misfits in their place
title_full Autofix for backward-fit sidechains: using MolProbity and real-space refinement to put misfits in their place
title_fullStr Autofix for backward-fit sidechains: using MolProbity and real-space refinement to put misfits in their place
title_full_unstemmed Autofix for backward-fit sidechains: using MolProbity and real-space refinement to put misfits in their place
title_short Autofix for backward-fit sidechains: using MolProbity and real-space refinement to put misfits in their place
title_sort autofix for backward-fit sidechains: using molprobity and real-space refinement to put misfits in their place
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2704614/
https://www.ncbi.nlm.nih.gov/pubmed/19002604
http://dx.doi.org/10.1007/s10969-008-9045-8
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