Contact Surface: Difference between revisions
Jump to navigation
Jump to search
No edit summary |
|||
(One intermediate revision by the same user not shown) | |||
Line 14: | Line 14: | ||
:: Note that this may be another protein! | :: Note that this may be another protein! | ||
'''states''' ''(integer)'', default:0 | '''states''' ''(integer)'', default:0 | ||
:: Calculate contact surface between the receptor and the first n states of the ligand. | :: Calculate contact surface between the receptor and the first n states of the ligand. | ||
Line 124: | Line 121: | ||
print "The contact areas between "+receptor+" and "+ligand+" [states 1 - "+str(states)+"] are (A^2):" | print "The contact areas between "+receptor+" and "+ligand+" [states 1 - "+str(states)+"] are (A^2):" | ||
#start looping | #start looping | ||
for s in range(1,states+1): | for s in range(1,states+1): | ||
#create complex | #create complex |
Latest revision as of 10:11, 15 February 2013
Overview
This script calculates individual or global contact areas between a receptor molecule and a (multimodel) bundle of docked ligand structures. The exact contact surface area values (in Angstrom^2) are printed to the screen and also appended to a file called contactareas.txt. If only a single global contact surface is calculated, a selection named "contact" is created that includes all receptor atoms within 3.9A of any ligand atom to illustrate the approximate contact surface.
The parameters are:
receptor (string)
- The name of the selection/object representing the receptor protein
ligand (string)
- The name of the selection/object representing the ligand
- Note that this may be another protein!
states (integer), default:0
- Calculate contact surface between the receptor and the first n states of the ligand.
- If states = 0, the script calculates a global contact surface which takes all possible ligand states into account.
Usage
contact_surface receptor, ligand, [states=0]
The Code
#contact_surface v.3.0
#Copyleft Martin Christen, 2013
from pymol import cmd,stored
def contact_surface(receptor,ligand,states=0):
"""
AUTHOR
Martin Christen
DESCRIPTION
This script calculates individual or global contact surfaces between a
receptor molecule and a bundle of docked ligand structures (which have
to be loaded into PyMOL as a multimodel object).
The exact contact surface area values (in Angstrom^2) are printed to
the screen and also appended to a file called contactareas.txt
If only a single global contact surface is calculated, a selection
named "contact" is created that includes all receptor atoms within
3.9A of any ligand atom.
USAGE
contact_surface receptor, ligand, [states=0]
PARAMETERS
receptor (string)
The name of the selection/object representing the receptor protein
ligand (string)
The name of the selection/object representing the ligand.
Note that this may be another protein!
states (integer)
Calculate contact surface between the receptor and the first n states
of the ligand. If states = 0 (default), the script calculates a global
contact surface which takes all possible ligand states into account.
"""
# sanity check the number of states
states = abs(int(states))
# make sure all atoms within an object occlude one another
cmd.flag('ignore','none')
# use solvent-accessible surface with high sampling density
cmd.set('dot_solvent','1')
cmd.set('dot_density','3')
#if the 'states' parameter = 0 create a superposition of all ligand states
if states == 0:
cmd.split_states(ligand)
cmd.group('ligandtemp',ligand+"_*")
cmd.create(ligand+"_all",'ligandtemp')
cmd.delete('ligandtemp')
#create complex
cmd.create('complextemp',ligand+"_all "+receptor)
#measure area
ligand_area=cmd.get_area(ligand+"_all")
receptor_area=cmd.get_area(receptor)
complex_area=cmd.get_area('complextemp')
#normalize since the area is counted TWICE (once on receptor and once on ligand)
contact_area=((ligand_area + receptor_area) - complex_area) / 2
#delete complex
cmd.delete('complextemp')
#create the contact surface
cmd.select('contact',"("+receptor+" and ("+ligand+"_all around 3.9))")
#print contact surface area
f=open('contactareas.txt','a')
print "%s - %s : " % (receptor,ligand),
print >>f, "%-s\t%-s\t" % (receptor,ligand),
print >>f, "%-s" % (contact_area)
print contact_area
f.close()
print "The GLOBAL contact area between "+receptor+ " and "+ligand+" is (A^2):"
print ((ligand_area + receptor_area) - complex_area) / 2
#If 'states' <> 0 calculate the contact areas to the first 'states' ligand states.
#No individual contact surface objects are created to avoid overloading PyMOL.
else:
#create an object for each ligand state
cmd.split_states(ligand)
#sanity check: do not exceed that maximum number of states
if states > cmd.count_states(ligand):
states = cmd.count_states(ligand)
#calculate contact surface area
print "The contact areas between "+receptor+" and "+ligand+" [states 1 - "+str(states)+"] are (A^2):"
#start looping
for s in range(1,states+1):
#create complex
cmd.create("tmp",ligand,s,1)
cmd.create('complextemp',"tmp "+receptor)
#measure areas
ligand_area=cmd.get_area('tmp')
receptor_area=cmd.get_area(receptor)
complex_area=cmd.get_area('complextemp')
#normalize since the area is counted TWICE (once on receptor and once on ligand)
contact_area=((ligand_area + receptor_area) - complex_area)/2
#delete temporary files
cmd.delete('tmp')
cmd.delete(ligand+"_*")
cmd.delete('complextemp')
#print contact surface area
f=open('contactareas.txt','a')
print "%s - %s_%-5s: " % (receptor,ligand,s),
print >>f, "%-s\t%-s_%-5s\t" % (receptor,ligand,s),
print >>f, "%-s" % (contact_area)
print contact_area
f.close()
cmd.extend("contact_surface",contact_surface)