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My name is Thomas Holder and I am a bioinformatician at the MPI for Developmental Biology in Tübingen, Germany.
My name is Thomas Holder and I worked on PyMOL for [https://www.schrodinger.com Schrödinger] 2012-2021.


=== Contact ===
I was awarded the [http://pymol.org/fellowship Warren L. DeLano Memorial PyMOL Open-Source Fellowship] for 2011-2012.


* speleo3/users.sourceforge.net
== Scripts written by me ==
* thomas.holder/tuebingen.mpg.de
 
=== Scripts written by me ===


* [[AAindex]]
* [[AAindex]]
* [[AngleBetweenHelices]]
* [[AngleBetweenHelices]]
* [[Extra fit]]
* [[PluginDirectory]]
* [[Pml2py]]
* [[Polarpairs]]
* [[Save settings]]
* [[Show bumps]]
* [[Sidechaincenters]]
* [[Sidechaincenters]]
* [[Spectrumany]]
* [[Spectrumany]]
* [[Spectrum states]]
* [[Supercell]]
* [[Supercell]]


=== Scripts Pastebin ===
== Scripts Pastebin ==


Some random scripts with no dedicated PyMOLWiki page.
Some random scripts with no dedicated PyMOLWiki page.
Launch interactive python terminal with PyMOL process:
(see also [[Launching From a Script]])


<source lang="python">
<source lang="python">
def extra_fit(selection='(all)', reference=None, method=cmd.align):
#!/usr/bin/ipython2.7 -i
     '''
 
DESCRIPTION
import threading
import pymol._cmd
 
pymol.invocation.parse_args(['pymol', '-qc'])
 
with threading.RLock():
    _COb = pymol._cmd._new(pymol, pymol.invocation.options)
     pymol._cmd._start(_COb, pymol.cmd)
    pymol.cmd._COb = _COb


    Like "intra_fit", but for multiple objects instead of
from pymol import cmd
    multiple states.
    '''
    models = cmd.get_object_list(selection)
    if reference is None:
        reference = models[0]
        models = models[1:]
    elif reference in models:
        models.remove(reference)
    if cmd.is_string(method):
        method = eval(method)
    for model in models:
        print model, method(model, reference)
cmd.extend('extra_fit', extra_fit)
</source>
</source>


<source lang="python">
<source lang="python">
def mse2met(selection='all', quiet=1):
#!/usr/bin/python2.6 -i
    '''
 
DESCRIPTION
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
</source>
 
Build FREEMOL (see also [[MovieSchool 6]])
 
<source lang="bash">
#!/bin/bash -e
 
src=/tmp
prefix=/opt/pymol-git
export FREEMOL=$prefix/freemol
 
freemoltrunk=$src/freemol-trunk
if [[ ! -e $freemoltrunk ]]; then
    svn co svn://bioinformatics.org/svnroot/freemol/trunk $freemoltrunk
fi
 
cd $freemoltrunk
 
sed -i 's/vdwtype\[11\]/vdwtype[14]/' src/mengine/src/field.h
 
for name in mpeg_encode mengine apbs pdb2pqr; do
    (cd src/$name && ./configure && make && make install)
done
 
cp -na freemol/libpy/freemol $prefix/modules/
 
ln -sfT $FREEMOL $prefix/modules/pymol/pymol_path/freemol
</source>
 
Download all PyMOL scripts from Robert L. Campbell's website:
 
<source lang="bash">
wget -r -np -nd --level=1 -A .py \
    http://pldserver1.biochem.queensu.ca/~rlc/work/pymol/
</source>
 
Render movie from PNG files (save as <code>png2mpeg1.sh</code>):
 
<source lang="bash">
#!/bin/bash
 
set -e
 
usage="usage: $(basename $0) [-w width] [-f fps] [-b vbitrate] <indir> <outfile.mpeg>"
width=""
fps=25
vbitrate=16000
 
args="$(getopt w:f:b:h "$@")" || args="-h"
set -- $args
 
while [[ $# > 0 ]]; do
    case "$1" in
        --) shift; break ;;
        -w) width=$2; shift 2 ;;
        -f) fps=$2; shift 2 ;;
        -b) vbitrate=$2; shift 2 ;;
        -h) echo $usage; exit 1 ;;
        *) echo "argument error: $1"; exit 1 ;;
    esac
done
 
if [[ $# > 2 ]]; then
    echo "too many arguments: $3 ..."
    echo $usage
    exit 1
fi


    Mutate selenomethionine to methionine
indir="$1"
    '''
outfile="$2"
    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):
if [[ -z "$indir" ]]; then
     '''
    echo "error: indir missing"
DESCRIPTION
    echo $usage
     exit 2
fi


     Remove alternative location atoms.
if [[ -z "$outfile" ]]; then
     echo "error: outfile missing"
    echo $usage
    exit 3
fi


ARGUMENTS
MENCODER="mencoder -quiet"
MPEG1ARGS="-mf type=png:fps=$fps -ovc lavc -forceidx -noskip \
    -of rawvideo -mpegopts format=mpeg1 \
    -lavcopts vcodec=mpeg1video:vbitrate=$vbitrate:vhq:trell:keyint=25"


     selection = string: atom selection
if [[ -n "$width" ]]; then
     MPEG1ARGS="-zoom -xy $width -sws 9 $MPEG1ARGS"
fi


    keep = string: AltLoc to keep {default: A}
pattern="mf://$indir/*.png"
    '''
$MENCODER "$pattern" $MPEG1ARGS:vpass=1 -o /dev/null
    cmd.remove('(%s) and not alt +%s' % (selection, keep), quiet=int(quiet))
$MENCODER "$pattern" $MPEG1ARGS:vpass=2 -o "$outfile"
    cmd.alter(selection, 'alt=""')
    cmd.sort()
cmd.extend('remove_alt', remove_alt)
</source>
</source>
=== Export movie with transparent background ===


<source lang="python">
<source lang="python">
def cbm(selection='(all)'):
# make transparent pngs
    '''
set opaque_background, off
DESCRIPTION
set ray_trace_frames
mpng foo
 
# create movie file (use codec "qtrle" or "png")
system ffmpeg -i foo%04d.png -vcodec qtrle foo.mov
 
# clean up
system rm -f foo????.png
</source>
 
=== load_mtz_cctbx: Load MTZ files with a [[CCTBX]] wrapper (3 files) ===
 
1) ~/bin/mtz2ccp4.sh


    Color by molecule
<source lang="bash">
    '''
#!/bin/bash
    col = 2
export PATH=/opt/ccp4/ccp4-6.5/bin:$PATH
    for model in cmd.get_object_list(selection):
exec cctbx.python ~/bin/mtz2ccp4.py "$@"
        cmd.color(col, '%s and (%s)' % (model, selection))
        col += 1
cmd.extend('cbm', cbm)
</source>
</source>
2) ~/bin/mtz2ccp4.py


<source lang="python">
<source lang="python">
def dev2b(selection='name CA'):
#!/opt/ccp4/ccp4-6.5/bin/cctbx.python
 
import os
import sys
import tempfile
 
def mtz2ccp4maps(filename, prefix='map'):
     '''
     '''
DESCRIPTION
Creates a temporary directory and dumps all maps from the given MTZ file
into this directory as CCP4 maps files. Returns the path of the temporary
directory.
    '''
    from iotbx.reflection_file_reader import any_reflection_file
 
    hkl_in = any_reflection_file(file_name=filename)
 
    temp_dir = tempfile.mkdtemp()
 
    for i_map, array in enumerate(hkl_in.as_miller_arrays()):
        if array.is_complex_array():
            fft_map = array.fft_map(resolution_factor=0.25).apply_sigma_scaling()
            map_filename = os.path.join(temp_dir,
                    prefix + '_' + '_'.join(array.info().labels) + '.ccp4')
            fft_map.as_ccp4_map(file_name=map_filename)
 
    return temp_dir


    Determine the RMSD per residue for a multi-state object and assign b-factor
# print the name of the temporary directory to standard output
    '''
print mtz2ccp4maps(*sys.argv[1:])
    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)
</source>
</source>
3) ~/.pymolrc.py


<source lang="python">
<source lang="python">
def select_extendbyss(selection, name=None, quiet=0):
@cmd.extend
def load_mtz_cctbx(filename, prefix=''):
     '''
     '''
DESCRIPTION
DESCRIPTION


     Extend selection by connected secondary structure elements.
     Load all maps from an MTZ file, using the mtz2ccp4.sh wrapper which
    uses iotbx (cctbx).
    '''
    import subprocess
    import glob
    import shutil


ARGUMENTS
    if not prefix:
        prefix = os.path.basename(filename).rpartition('.')[0]
 
    outdir = subprocess.Popen([os.path.expanduser('~/bin/mtz2ccp4.sh'),
        filename, prefix], stdout=subprocess.PIPE).stdout.readlines()[0].strip()


     selection = string: selection-expression
     for mapfilename in glob.glob(os.path.join(outdir, '*.ccp4')):
        cmd.load(mapfilename)


     name = string: create a named atom selection if not None {default: None}
     shutil.rmtree(outdir)
    '''
    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)
</source>
</source>
=== ccmutate ===


<source lang="python">
<source lang="python">
def diff(sele1, sele2, byres=1, name=None, operator='in', quiet=0):
@cmd.extend
def ccmutate(code, selection='??sele|?pk1', sculpt=1):
     '''
     '''
DESCRIPTION
DESCRIPTION


     Difference between two molecules
     Mutate selected residue.


ARGUMENTS
ARGUMENTS


     sele1 = string: atom selection
     code = str: 3-letter PDBeChem chemical component identifier


     sele2 = string: atom selection
     selection = str: single residue selection {default: pk1 or sele}


     byres = 0/1: report residues, not atoms (does not affect selection)
     sculpt = 0/1: try to adopt conformation of replaced sidechain, followed
     {default: 1}
     by relaxation using sculpting {default: 1}


     operator = in/like/align: operator to match atoms {default: in}
EXAMPLE
 
     fetch 1ubq, async=0
    ccmutate 0HG, resi 24


SEE ALSO
SEE ALSO


     symdiff
     fetch ..., type=cc
    wizard mutagenesis
     '''
     '''
     byres, quiet = int(byres), int(quiet)
     code = code.upper()
    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):
    tmp_sele = cmd.get_unused_name('_sele')
    '''
    tmp_frag = cmd.get_unused_name('_frag')
DESCRIPTION
    tmp_Nnbr = cmd.get_unused_name('_Nnbr')
    tmp_back = cmd.get_unused_name('_back')
    tmp_tmpl = cmd.get_unused_name('_tmpl')
    tmp_sc_o = cmd.get_unused_name('_sc_o')
    tmp_sc_n = cmd.get_unused_name('_sc_n')
 
    try:
        cmd.select(tmp_sele, 'byres (' + selection + ')', 0)
 
        # check input selection
        if cmd.count_atoms('name CA & ?' + tmp_sele) != 1:
            raise pymol.CmdException('selection must include exactly one residue')
        if cmd.count_atoms('name N+CA+C & ?' + tmp_sele) != 3:
            raise pymol.CmdException("selected residue doesn't have N+CA+C atoms")
 
        # PDBeChem fragment
        cmd.fetch(code, tmp_frag, type='cc', zoom=0)
 
        # check if fragment is amino acid
        if cmd.count_atoms('name N+CA+C & ?' + tmp_frag) != 3:
            raise pymol.CmdException("residue '%s' doesn't have N+CA+C atoms" % (code))
 
        # only keep hydrogens if target also has hydrogens
        if cmd.count_atoms('hydro & ?' + tmp_sele) == 0:
            cmd.remove('hydro & ?' + tmp_frag)
 
        # update residue name for old residue
        cmd.alter(tmp_sele, 'resn = ' + repr(code))
 
        # superpose fragment on backbone
        cmd.align(
                'name N+CA+C & ?' + tmp_frag,
                'name N+CA+C & ?' + tmp_sele)
 
        # extra N bonds, like in PRO
        cmd.select(tmp_Nnbr, 'neighbor (name N & ?' + tmp_frag + ')', 0)
 
        # backbone selection
        cmd.select(tmp_back, 'name CA+C+O+N+OXT', 0)
        cmd.select(tmp_back, 'hydro & neighbor ?' + tmp_back, 0, merge=1)
 
        # remove complementary atoms
        cmd.remove(          '?' + tmp_frag + ' & ' + tmp_back)
        cmd.extract(tmp_tmpl, '?' + tmp_sele + ' & !' + tmp_back, zoom=0)
 
        if cmd.count_atoms(tmp_frag):
            # attach new sidechain
            cmd.fuse('name CB & ?' + tmp_frag, 'name CA & ?' + tmp_sele, mode=1, move=0)
            cmd.unpick()
 
            # new atom selections
            cmd.select(tmp_sc_n, '(byres ?' + tmp_sele + ') & !?' + tmp_sele, 0)
            cmd.select(tmp_sc_o, '?' + tmp_sc_n + ' like ?' + tmp_tmpl, 0)
 
            # extra N bonds, like in PRO
            if cmd.count_atoms(tmp_Nnbr):
                cmd.bond('?' + tmp_sc_n + ' like ?' + tmp_Nnbr, 'name N & ?' + tmp_sele)


    Symmetric difference between two molecules
            # adopt old conformation, if possible
            if int(sculpt):
                model = cmd.get_object_list('?' + tmp_sele)[0]
                cmd.protect(model)
                cmd.deprotect('?' + tmp_sc_n + ' & !?' + tmp_sc_o)
                cmd.sculpt_activate(model)
                if cmd.count_atoms(tmp_sc_o):
                    cmd.update(tmp_sc_o, tmp_tmpl)
                    cmd.set('sculpt_field_mask', 63) # local geom + vdw
                    cmd.sculpt_iterate(model, cycles=100)
                    cmd.deprotect(tmp_sc_o)
                cmd.set('sculpt_field_mask', 0xff) # all
                cmd.sculpt_iterate(model, cycles=200)
                cmd.set('sculpt_field_mask', 31) # local geom
                cmd.sculpt_iterate(model, cycles=200)


SEE ALSO
    finally:
        cmd.delete(tmp_sele)
        cmd.delete(tmp_frag)
        cmd.delete(tmp_Nnbr)
        cmd.delete(tmp_back)
        cmd.delete(tmp_tmpl)
        cmd.delete(tmp_sc_o)
        cmd.delete(tmp_sc_n)
</source>


    diff
=== CTRL-L ligand zoom ===
    '''
    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)
<source lang="python">
cmd.extend('diff', diff)
@cmd.set_key('CTRL-L')
def ligand_zoom():
    global _current_ligand
    s = {'ligand_set': set()}
    if cmd.iterate('organic', 'ligand_set.add((model,segi,chain,resi))',
            space=s) < 1:
        return
    ligands = sorted(s["ligand_set"])
    try:
        i = ligands.index(_current_ligand)
    except (ValueError, NameError):
        i = -1
    i = (i + 1) % len(ligands)
    _current_ligand = ligands[i]
    # use "do" for feedback
    cmd.do('zoom /%s/%s/%s & resi %s, animate=1, buffer=2' % ligands[i])
</source>
</source>
=== Compile on FreeBSD ===
pkg upgrade
pkg install subversion py27-Pmw glew freeglut png freetype2 libxml2 msgpack
python2 setup.py install --prefix=$HOME/opt/pymol-svn

Latest revision as of 16:55, 23 November 2021

My name is Thomas Holder and I worked on PyMOL for Schrödinger 2012-2021.

I was awarded the Warren L. DeLano Memorial PyMOL Open-Source Fellowship for 2011-2012.

Scripts written by me

Scripts Pastebin

Some random scripts with no dedicated PyMOLWiki page.

Launch interactive python terminal with PyMOL process: (see also Launching From a Script)

#!/usr/bin/ipython2.7 -i

import threading
import pymol._cmd

pymol.invocation.parse_args(['pymol', '-qc'])

with threading.RLock():
    _COb = pymol._cmd._new(pymol, pymol.invocation.options)
    pymol._cmd._start(_COb, pymol.cmd)
    pymol.cmd._COb = _COb

from pymol import cmd
#!/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 FREEMOL (see also MovieSchool 6)

#!/bin/bash -e

src=/tmp
prefix=/opt/pymol-git
export FREEMOL=$prefix/freemol

freemoltrunk=$src/freemol-trunk
if [[ ! -e $freemoltrunk ]]; then
    svn co svn://bioinformatics.org/svnroot/freemol/trunk $freemoltrunk
fi

cd $freemoltrunk

sed -i 's/vdwtype\[11\]/vdwtype[14]/' src/mengine/src/field.h

for name in mpeg_encode mengine apbs pdb2pqr; do
    (cd src/$name && ./configure && make && make install)
done

cp -na freemol/libpy/freemol $prefix/modules/

ln -sfT $FREEMOL $prefix/modules/pymol/pymol_path/freemol

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/

Render movie from PNG files (save as png2mpeg1.sh):

#!/bin/bash

set -e

usage="usage: $(basename $0) [-w width] [-f fps] [-b vbitrate] <indir> <outfile.mpeg>"
width=""
fps=25
vbitrate=16000

args="$(getopt w:f:b:h "$@")" || args="-h"
set -- $args

while [[ $# > 0 ]]; do
    case "$1" in
        --) shift; break ;;
        -w) width=$2; shift 2 ;;
        -f) fps=$2; shift 2 ;;
        -b) vbitrate=$2; shift 2 ;;
        -h) echo $usage; exit 1 ;;
        *) echo "argument error: $1"; exit 1 ;;
    esac
done

if [[ $# > 2 ]]; then
    echo "too many arguments: $3 ..."
    echo $usage
    exit 1
fi

indir="$1"
outfile="$2"

if [[ -z "$indir" ]]; then
    echo "error: indir missing"
    echo $usage
    exit 2
fi

if [[ -z "$outfile" ]]; then
    echo "error: outfile missing"
    echo $usage
    exit 3
fi

MENCODER="mencoder -quiet"
MPEG1ARGS="-mf type=png:fps=$fps -ovc lavc -forceidx -noskip \
    -of rawvideo -mpegopts format=mpeg1 \
    -lavcopts vcodec=mpeg1video:vbitrate=$vbitrate:vhq:trell:keyint=25"

if [[ -n "$width" ]]; then
    MPEG1ARGS="-zoom -xy $width -sws 9 $MPEG1ARGS"
fi

pattern="mf://$indir/*.png"
$MENCODER "$pattern" $MPEG1ARGS:vpass=1 -o /dev/null
$MENCODER "$pattern" $MPEG1ARGS:vpass=2 -o "$outfile"

Export movie with transparent background

# make transparent pngs
set opaque_background, off
set ray_trace_frames
mpng foo

# create movie file (use codec "qtrle" or "png")
system ffmpeg -i foo%04d.png -vcodec qtrle foo.mov 

# clean up
system rm -f foo????.png

load_mtz_cctbx: Load MTZ files with a CCTBX wrapper (3 files)

1) ~/bin/mtz2ccp4.sh

#!/bin/bash
export PATH=/opt/ccp4/ccp4-6.5/bin:$PATH
exec cctbx.python ~/bin/mtz2ccp4.py "$@"

2) ~/bin/mtz2ccp4.py

#!/opt/ccp4/ccp4-6.5/bin/cctbx.python

import os
import sys
import tempfile

def mtz2ccp4maps(filename, prefix='map'):
    '''
Creates a temporary directory and dumps all maps from the given MTZ file
into this directory as CCP4 maps files. Returns the path of the temporary
directory.
    '''
    from iotbx.reflection_file_reader import any_reflection_file

    hkl_in = any_reflection_file(file_name=filename)

    temp_dir = tempfile.mkdtemp()

    for i_map, array in enumerate(hkl_in.as_miller_arrays()):
        if array.is_complex_array():
            fft_map = array.fft_map(resolution_factor=0.25).apply_sigma_scaling()
            map_filename = os.path.join(temp_dir,
                    prefix + '_' + '_'.join(array.info().labels) + '.ccp4')
            fft_map.as_ccp4_map(file_name=map_filename)

    return temp_dir

# print the name of the temporary directory to standard output
print mtz2ccp4maps(*sys.argv[1:])

3) ~/.pymolrc.py

@cmd.extend
def load_mtz_cctbx(filename, prefix=''):
    '''
DESCRIPTION

    Load all maps from an MTZ file, using the mtz2ccp4.sh wrapper which
    uses iotbx (cctbx).
    '''
    import subprocess
    import glob
    import shutil

    if not prefix:
        prefix = os.path.basename(filename).rpartition('.')[0]

    outdir = subprocess.Popen([os.path.expanduser('~/bin/mtz2ccp4.sh'),
        filename, prefix], stdout=subprocess.PIPE).stdout.readlines()[0].strip()

    for mapfilename in glob.glob(os.path.join(outdir, '*.ccp4')):
        cmd.load(mapfilename)

    shutil.rmtree(outdir)

ccmutate

@cmd.extend
def ccmutate(code, selection='??sele|?pk1', sculpt=1):
    '''
DESCRIPTION

    Mutate selected residue.

ARGUMENTS

    code = str: 3-letter PDBeChem chemical component identifier

    selection = str: single residue selection {default: pk1 or sele}

    sculpt = 0/1: try to adopt conformation of replaced sidechain, followed
    by relaxation using sculpting {default: 1}

EXAMPLE

    fetch 1ubq, async=0
    ccmutate 0HG, resi 24

SEE ALSO

    fetch ..., type=cc
    wizard mutagenesis
    '''
    code = code.upper()

    tmp_sele = cmd.get_unused_name('_sele')
    tmp_frag = cmd.get_unused_name('_frag')
    tmp_Nnbr = cmd.get_unused_name('_Nnbr')
    tmp_back = cmd.get_unused_name('_back')
    tmp_tmpl = cmd.get_unused_name('_tmpl')
    tmp_sc_o = cmd.get_unused_name('_sc_o')
    tmp_sc_n = cmd.get_unused_name('_sc_n')

    try:
        cmd.select(tmp_sele, 'byres (' + selection + ')', 0)

        # check input selection
        if cmd.count_atoms('name CA & ?' + tmp_sele) != 1:
            raise pymol.CmdException('selection must include exactly one residue')
        if cmd.count_atoms('name N+CA+C & ?' + tmp_sele) != 3:
            raise pymol.CmdException("selected residue doesn't have N+CA+C atoms")

        # PDBeChem fragment
        cmd.fetch(code, tmp_frag, type='cc', zoom=0)

        # check if fragment is amino acid
        if cmd.count_atoms('name N+CA+C & ?' + tmp_frag) != 3:
            raise pymol.CmdException("residue '%s' doesn't have N+CA+C atoms" % (code))

        # only keep hydrogens if target also has hydrogens
        if cmd.count_atoms('hydro & ?' + tmp_sele) == 0:
            cmd.remove('hydro & ?' + tmp_frag)

        # update residue name for old residue
        cmd.alter(tmp_sele, 'resn = ' + repr(code))

        # superpose fragment on backbone
        cmd.align(
                'name N+CA+C & ?' + tmp_frag,
                'name N+CA+C & ?' + tmp_sele)

        # extra N bonds, like in PRO
        cmd.select(tmp_Nnbr, 'neighbor (name N & ?' + tmp_frag + ')', 0)

        # backbone selection
        cmd.select(tmp_back, 'name CA+C+O+N+OXT', 0)
        cmd.select(tmp_back, 'hydro & neighbor ?' + tmp_back, 0, merge=1)

        # remove complementary atoms
        cmd.remove(           '?' + tmp_frag + ' & ' + tmp_back)
        cmd.extract(tmp_tmpl, '?' + tmp_sele + ' & !' + tmp_back, zoom=0)

        if cmd.count_atoms(tmp_frag):
            # attach new sidechain
            cmd.fuse('name CB & ?' + tmp_frag, 'name CA & ?' + tmp_sele, mode=1, move=0)
            cmd.unpick()

            # new atom selections
            cmd.select(tmp_sc_n, '(byres ?' + tmp_sele + ') & !?' + tmp_sele, 0)
            cmd.select(tmp_sc_o, '?' + tmp_sc_n + ' like ?' + tmp_tmpl, 0)

            # extra N bonds, like in PRO
            if cmd.count_atoms(tmp_Nnbr):
                cmd.bond('?' + tmp_sc_n + ' like ?' + tmp_Nnbr, 'name N & ?' + tmp_sele)

            # adopt old conformation, if possible
            if int(sculpt):
                model = cmd.get_object_list('?' + tmp_sele)[0]
                cmd.protect(model)
                cmd.deprotect('?' + tmp_sc_n + ' & !?' + tmp_sc_o)
                cmd.sculpt_activate(model)
                if cmd.count_atoms(tmp_sc_o):
                    cmd.update(tmp_sc_o, tmp_tmpl)
                    cmd.set('sculpt_field_mask', 63) # local geom + vdw
                    cmd.sculpt_iterate(model, cycles=100)
                    cmd.deprotect(tmp_sc_o)
                cmd.set('sculpt_field_mask', 0xff) # all
                cmd.sculpt_iterate(model, cycles=200)
                cmd.set('sculpt_field_mask', 31) # local geom
                cmd.sculpt_iterate(model, cycles=200)

    finally:
        cmd.delete(tmp_sele)
        cmd.delete(tmp_frag)
        cmd.delete(tmp_Nnbr)
        cmd.delete(tmp_back)
        cmd.delete(tmp_tmpl)
        cmd.delete(tmp_sc_o)
        cmd.delete(tmp_sc_n)

CTRL-L ligand zoom

@cmd.set_key('CTRL-L')
def ligand_zoom():
    global _current_ligand
    s = {'ligand_set': set()}
    if cmd.iterate('organic', 'ligand_set.add((model,segi,chain,resi))',
            space=s) < 1:
        return
    ligands = sorted(s["ligand_set"])
    try:
        i = ligands.index(_current_ligand)
    except (ValueError, NameError):
        i = -1
    i = (i + 1) % len(ligands)
    _current_ligand = ligands[i]
    # use "do" for feedback
    cmd.do('zoom /%s/%s/%s & resi %s, animate=1, buffer=2' % ligands[i])

Compile on FreeBSD

pkg upgrade
pkg install subversion py27-Pmw glew freeglut png freetype2 libxml2 msgpack
python2 setup.py install --prefix=$HOME/opt/pymol-svn