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Docking configuration files for all-atom and coarse-grained pipeline #2

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65 changes: 65 additions & 0 deletions haddock3-scripts/docking-unbound_benchmark_AA.cfg
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Original file line number Diff line number Diff line change
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# ====================================================================
# Protein-DNA docking benchmark configuration file
# ====================================================================

# directory in which docking will be done
run_dir = run-AA-XX

# execution mode
mode = "local"
ncores = 80
debug = true

# molecules to be docked
molecules = [
"XX_p?_u.pdb",
"XX_d_u.pdb"
]



# ====================================================================
# Parameters for each stage are defined below; prefer full paths
# ====================================================================

[topoaa]

[rigidbody]
tolerance = 90
ambig_fname = "XX_u_ambig.tbl"
sampling = 1000
epsilon = 78
dielec = "cdie"
w_desolv = 0

[caprieval]
reference_fname = "XX_target.pdb"

[seletop]
select = 200

[flexref]
tolerance = 90
ambig_fname = "XX_u_ambig.tbl"
epsilon = 78
dielec = "cdie"
dnarest_on = true
w_desolv = 0

[caprieval]
reference_fname = "XX_target.pdb"

[emref]
ambig_fname = "XX_u_ambig.tbl"
dnarest_on = true
w_desolv = 0

[caprieval]
reference_fname = "XX_target.pdb"

[clustfcc]

[seletopclusts]

[caprieval]
reference_fname = "XX_target.pdb"
72 changes: 72 additions & 0 deletions haddock3-scripts/docking-unbound_benchmark_CG.cfg
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Original file line number Diff line number Diff line change
@@ -0,0 +1,72 @@
# ====================================================================
# Protein-DNA docking benchmark configuration file
# ====================================================================

# directory in which docking will be done
run_dir = run-CG-XX

# execution mode
mode = "local"
ncores = 80
debug = true

# molecules to be docked
molecules = [
"XX_p?_u.pdb",
"XX_d_u.pdb"
]



# ====================================================================
# Parameters for each stage are defined below; prefer full paths
# ====================================================================

[topoaa]

[topocg]
cgffversion = "martini2"

[rigidbody]
tolerance = 90
ambig_fname = "XX_u_ambig.tbl"
epsilon = 78
dielec = "cdie"
w_desolv = 0
sampling = 1000

[caprieval]
fnat_cutoff = 7.0 # CG cutoff
reference_fname = "XX_target.pdb"

[seletop]
select = 200

[flexref]
tolerance = 90
ambig_fname = "XX_u_ambig.tbl"
epsilon = 78
dielec = "cdie"
dnarest_on = true
w_desolv = 0

[caprieval]
fnat_cutoff = 7.0 # CG cutoff
reference_fname = "XX_target.pdb"

[cgtoaa]

[emref]
ambig_fname = "XX_u_ambig.tbl"
dnarest_on = true
w_desolv = 0

[caprieval]
reference_fname = "XX_target.pdb"

[clustfcc]

[seletopclusts]

[caprieval]
reference_fname = "XX_target.pdb"