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Blind Test of Physics-Based Prediction of Protein Structures

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1 Blind Test of Physics-Based Prediction of Protein Structures
M. Scott Shell, S. Banu Ozkan, Vincent Voelz, Guohong Albert Wu, Ken A. Dill  Biophysical Journal  Volume 96, Issue 3, Pages (February 2009) DOI: /j.bpj Copyright © 2009 Biophysical Society Terms and Conditions

2 Figure 1 Folding routes found in the ZAM conformational search process for the CASP7 target T0358. Residue number ranges are shown below fragments. Only a subset of all steps and pathways is shown. ZAM begins by dividing the full chain into overlapping 8-mer fragments, spaced every three residues. These 8-mer fragments are grown over several stages to 16–20 mers; each stage involves adding new terminal residues to the structures followed by REMD sampling. Subsequently, secondary structure pieces neighboring in sequence are assembled together in various combinations using rigid-body alignment, followed by additional REMD sampling. The process continues along all possible pathways until a full fold is reached. Some assembly steps fail, resulting in loss of previous developed structure (31–70), whereas others cannot be assembled or grown so as to form new secondary structure later on (57–87)—those pathways are not pursued further. Along any one pathway, harmonic restraints are used to reinforce stable hydrophobic-hydrophobic contacts in the fragments and to avoid resampling existing structure. Colors in the fragments are as follows: green, hydrophobic; gray, polar; red, acidic; blue, basic. Biophysical Journal  , DOI: ( /j.bpj ) Copyright © 2009 Biophysical Society Terms and Conditions

3 Figure 2 Number of fragments simulated during ZAM as a function of fragment length, for the target T0358. The high number of fragments at lengths of 70+ residues corresponds to the generation of different topologies from the assembly of two fragments of shorter lengths. Biophysical Journal  , DOI: ( /j.bpj ) Copyright © 2009 Biophysical Society Terms and Conditions

4 Figure 3 ZAM predictions in CASP7 compared with experimental PDB structures. The CASP GDT gives the percentage of residues (x axis) whose Cα coordinates lie within a given cutoff distance (y axis) from the native structure, for predictions by all participants in CASP7 (orange colors). The best predictions correspond to lines in the lower-right quadrant of the graph. The five ZAM models are shown for each target in gray, with the structural model shown highlighted in red. Biophysical Journal  , DOI: ( /j.bpj ) Copyright © 2009 Biophysical Society Terms and Conditions

5 Figure 4 Secondary structure analysis of ZAM predictions. The first line for each target gives the DSSP-computed (39) secondary structure; the bottom line gives the same for the native structure. Residues not solved in the native structure are indicated by X. Biophysical Journal  , DOI: ( /j.bpj ) Copyright © 2009 Biophysical Society Terms and Conditions

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