User:Speleo3
Jump to navigation
Jump to search
My name is Thomas Holder and I am a bioinformatician at the MPI for Developmental Biology in Tübingen, Germany.
I was awarded the Warren L. DeLano Memorial PyMOL Open-Source Fellowship for 2011-2012.
Contact
- speleo3/users.sourceforge.net
- thomas.holder/tuebingen.mpg.de
Scripts written by me
- AAindex
- AngleBetweenHelices
- Extra fit
- PluginDirectory
- Pml2py
- Polarpairs
- Save settings
- Show bumps
- Sidechaincenters
- Spectrumany
- Spectrum states
- Supercell
Scripts Pastebin
Some random scripts with no dedicated PyMOLWiki page.
def mse2met(selection='all', quiet=1):
'''
DESCRIPTION
Mutate selenomethionine to methionine
'''
quiet = int(quiet)
x = cmd.alter('(%s) and MSE/SE' % selection, 'name="SD";elem="S"')
cmd.alter('(%s) and MSE/' % selection, 'resn="MET";type="ATOM"')
if not quiet:
print 'Altered %d MSE residues to MET' % (x)
cmd.sort()
cmd.extend('mse2met', mse2met)
def remove_alt(selection='all', keep='A', quiet=1):
'''
DESCRIPTION
Remove alternative location atoms.
ARGUMENTS
selection = string: atom selection
keep = string: AltLoc to keep {default: A}
'''
cmd.remove('(%s) and not alt +%s' % (selection, keep), quiet=int(quiet))
cmd.alter(selection, 'alt=""')
cmd.sort()
cmd.extend('remove_alt', remove_alt)
def cbm(selection='(all)'):
'''
DESCRIPTION
Color by molecule
'''
col = 2
for model in cmd.get_object_list(selection):
cmd.color(col, '%s and (%s)' % (model, selection))
col += 1
cmd.extend('cbm', cbm)
def dev2b(selection='name CA'):
'''
DESCRIPTION
Determine the RMSD per residue for a multi-state object and assign b-factor
'''
import numpy
stored.x = dict()
stored.b = dict()
for state in range(1, cmd.count_states()+1):
cmd.iterate_state(state, selection, 'stored.x.setdefault((model,segi,chain,resi,name), []).append([x,y,z])')
for key, coord_list in stored.x.iteritems():
b_sq = numpy.array(coord_list).var(0).mean() # var over states, mean over x,y,z
stored.b[key] = numpy.sqrt(b_sq) * 10.0
cmd.alter(selection, 'b = stored.b[model,segi,chain,resi,name]')
cmd.extend('dev2b', dev2b)
def select_extendbyss(selection, name=None, quiet=0):
'''
DESCRIPTION
Extend selection by connected secondary structure elements.
ARGUMENTS
selection = string: selection-expression
name = string: create a named atom selection if not None {default: None}
'''
def in_intervals(i, intervals):
for interval in intervals:
if interval[0] <= i and i <= interval[1]:
return True
return False
quiet = int(quiet)
stored.x = set()
# only iterate over CAs since for example PyMOL's dss command just
# assignes ss to CAs.
cmd.iterate('bycalpha (%s)' % (selection),
'stored.x.add((model,segi,chain,resv,ss))')
elements = dict()
for model,segi,chain,resv,ss in stored.x:
key = (model,segi,chain,ss)
elements.setdefault(key, [])
if in_intervals(resv, elements[key]):
continue
stored.b = set()
cmd.iterate('/%s/%s/%s//CA and ss "%s"' % key, 'stored.b.add(resv)')
resv_min = resv
resv_max = resv
while (resv_min - 1) in stored.b:
resv_min -= 1
while (resv_max + 1) in stored.b:
resv_max += 1
elements[key].append((resv_min, resv_max))
sele_list = []
ss_names = {'S': 'Strand', 'H': 'Helix', '': 'Loop'}
for key in elements:
model,segi,chain,ss = key
for resv_min,resv_max in elements[key]:
sele = '/%s/%s/%s/%d-%d' % (model, segi, chain, resv_min, resv_max)
sele_list.append(sele)
if not quiet:
print ss_names.get(ss, ss), sele
sele = ' or '.join(sele_list)
if name is not None:
cmd.select(name, sele)
if not quiet:
print 'Selection:', sele
return sele
cmd.extend('select_extendbyss', select_extendbyss)
def diff(sele1, sele2, byres=1, name=None, operator='in', quiet=0):
'''
DESCRIPTION
Difference between two molecules
ARGUMENTS
sele1 = string: atom selection
sele2 = string: atom selection
byres = 0/1: report residues, not atoms (does not affect selection)
{default: 1}
operator = in/like/align: operator to match atoms {default: in}
SEE ALSO
symdiff
'''
byres, quiet = int(byres), int(quiet)
if name is None:
name = cmd.get_unused_name('diff')
if operator == 'align':
alnobj = cmd.get_unused_name('__aln')
cmd.align(sele1, sele2, cycles=0, transform=0, object=alnobj)
sele = '(%s) and not %s' % (sele1, alnobj)
cmd.select(name, sele)
cmd.delete(alnobj)
else:
sele = '(%s) and not ((%s) %s (%s))' % (sele1, sele1, operator, sele2)
cmd.select(name, sele)
if not quiet:
if byres:
seleiter = 'byca ' + name
expr = 'print "/%s/%s/%s/%s`%s" % (model,segi,chain,resn,resi)'
else:
seleiter = name
expr = 'print "/%s/%s/%s/%s`%s/%s" % (model,segi,chain,resn,resi,name)'
cmd.iterate(seleiter, expr)
return name
def symdiff(sele1, sele2, byres=1, name=None, operator='in', quiet=0):
'''
DESCRIPTION
Symmetric difference between two molecules
SEE ALSO
diff
'''
byres, quiet = int(byres), int(quiet)
if name is None:
name = cmd.get_unused_name('symdiff')
tmpname = cmd.get_unused_name('__tmp')
diff(sele1, sele2, byres, name, operator, quiet)
diff(sele2, sele1, byres, tmpname, operator, quiet)
cmd.select(name, tmpname, merge=1)
cmd.delete(tmpname)
return name
cmd.extend('symdiff', symdiff)
cmd.extend('diff', diff)
Launch interactive python terminal with PyMOL process: (see also Launching From a Script)
#!/usr/bin/python2.6 -i
import sys, os
# autocompletion
import readline
import rlcompleter
readline.parse_and_bind('tab: complete')
# pymol environment
moddir='/opt/pymol-svn/modules'
sys.path.insert(0, moddir)
os.putenv('PYMOL_PATH', os.path.join(moddir, 'pymol/pymol_path'))
# pymol launching
import pymol
pymol.pymol_argv = ['pymol','-qc'] + sys.argv[1:]
pymol.finish_launching()
cmd = pymol.cmd
Build PyMOL: (see also Linux Install)
#!/bin/bash -e
prefix=/opt/pymol-svn
modules=$prefix/modules
python setup.py build install \
--home=$prefix \
--install-purelib=$modules \
--install-platlib=$modules
export PYTHONPATH=$modules:$PYTHONPATH
python setup2.py install
install pymol $prefix/
Download all PyMOL scripts from Robert L. Campbell's website:
wget -r -np -nd --level=1 -A .py \
http://pldserver1.biochem.queensu.ca/~rlc/work/pymol/