Coarse- and fine-grained models for proteins: Evaluation by decoy discrimination

Chris Kauffman, George Karypis

Research output: Contribution to journalArticlepeer-review

1 Scopus citations

Abstract

Coarse-grained models for protein structure are increasingly used in simulations and structural bioinformatics. In this study, we evaluated the effectiveness of three granularities of protein representation based on their ability to discriminate between correctly folded native structures and incorrectly folded decoy structures. The three levels of representation used one bead per amino acid (coarse), two beads per amino acid (medium), and all atoms (fine). Multiple structure features were compared at each representation level including two-body interactions, three-body interactions, solvent exposure, contact numbers, and angle bending. In most cases, the all-atom level was most successful at discriminating decoys, but the two-bead level provided a good compromise between the number of model parameters which must be estimated and the accuracy achieved. The most effective feature type appeared to be two-body interactions. Considering three-body interactions increased accuracy only marginally when all atoms were used and not at all in medium and coarse representations. Though two-body interactions were most effective for the coarse representations, the accuracy loss for using only solvent exposure or contact number was proportionally less at these levels than in the all-atom representation. We propose an optimization method capable of selecting bead types of different granularities to create a mixed representation of the protein. We illustrate its behavior on decoy discrimination and discuss implications for data-driven protein model selection.

Original languageEnglish (US)
Pages (from-to)754-773
Number of pages20
JournalProteins: Structure, Function and Bioinformatics
Volume81
Issue number5
DOIs
StatePublished - May 1 2013

Keywords

  • Coarse-grained models
  • Machine learning
  • N-body interactions
  • Protein decoy discrimination
  • Protein model selection

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