Difference between revisions of "Workflow homology modelling glucocerebrosidase"
From Bioinformatikpedia
(→Preparation of the Alignment File) |
(→Modelling of the Target Structure) |
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#: Note that all files (alignment- and structure file) must be in the same folder |
#: Note that all files (alignment- and structure file) must be in the same folder |
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<code> |
<code> |
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| − | from modeller.automodel import * |
+ | from modeller.automodel import * |
| − | log.verbose() |
+ | log.verbose() |
| − | env = environ() |
+ | env = environ() |
| − | env.io.atom_files_directory = '' |
+ | env.io.atom_files_directory = '' |
| − | a = automodel (env, alnfile = ' |
+ | a = automodel (env, alnfile = 'TARGET_TEMPLATE.ali', knowns = 'TEMPLATE', sequence = 'TARGET') |
| − | a.starting_model = 1 |
+ | a.starting_model = 1 |
| − | a.ending_model = 1 |
+ | a.ending_model = 1 |
| − | a.make() |
+ | a.make() |
</code> |
</code> |
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Revision as of 11:58, 11 June 2011
Detailed workflow of the different homology modelling approaches for glucocerebrosidase. Return to overview.
Contents
MODELLER
Preparation of the Alignment File
- Save target protein sequence in PIR-format: target.pir
- Save PDB-file of template sequence: template:pdb
- If PDB-file consists of several chains: split pdb file with the help of splitpdb (note that minor changes are needed, so that ATOM coordinates get listed in the resulting PDB-file instead of HETATOMS).
- Run the following Python script with command '
mod9.9 align.py' to create a target-template alignment in PIR-format:
log.verbose()
env = environ()
aln = alignment(env)
mdl= model(env, file='template')
aln.append_model(mdl, align_codes='template')
aln.append(file='target.pir', align_codes=('target'))
aln.align(gap_penalties_1d=(-600,-400))
aln.write(file='target_template.ali', alignment_format='PIR')
aln.write(file='target_template.pap', alignment_format='PAP')
Modelling of the Target Structure
- Run the following Python script with command '
mod9.9 model.py' to model the structure of the target sequence:- Note that all files (alignment- and structure file) must be in the same folder
from modeller.automodel import *
log.verbose()
env = environ()
env.io.atom_files_directory =
a = automodel (env, alnfile = 'TARGET_TEMPLATE.ali', knowns = 'TEMPLATE', sequence = 'TARGET')
a.starting_model = 1
a.ending_model = 1
a.make()
I-TASSER
- Webserver: http://zhanglab.ccmb.med.umich.edu/I-TASSER/
- Input: protein sequence in FASTA-format.
SWISS-MODELLER
Automated Mode
- Webserver: http://swissmodel.expasy.org/workspace/index.php?func=modelling_simple1
- Input: Sequence in fasta format
The automated mode should only be used, if target and template share more than 50% of sequence identity.
Alignment Mode
- Webserver: http://swissmodel.expasy.org/workspace/index.php?func=modelling_align1
- Input: Target-Template Alignment in different formats (FASTA, CLUSTALW, ...)
To create the Alignments needed as input, the tool ClustalW2 was used in this case.
