Difference between revisions of "User talk:Remig"

From Jmol
Jump to navigation Jump to search
(Ribozome - an Alpha Helix Generator)
(Replaced content with "What I had here before belongs on the user page - so I moved it...")
 
(5 intermediate revisions by the same user not shown)
Line 1: Line 1:
I use Jmol to study protein folding. Here is a script I wrote that accepts an amino acid sequence (1 letter encoding: "AAC...FYW" for example) and generates an alpha helix using the Model Kit:
+
What I had here before belongs on the user page - so I moved it...
<pre># RIBOZOME - Jmol script by Ron Mignery
 
# v1.0 beta 10/19/2013
 
#
 
# RIBOZOME takes a string message encoding an amino acid (aa) sequence
 
# and generates a corresponding alpha helix one aa at a time from the
 
# N terminus to the C terminus rotating the emerging helix as it goes.
 
#
 
# The message is a string entered by the user at a prompt.
 
# It may be typed in or pasted in and be of any length
 
#
 
# The IUPAC/IUBMB 1 letter code is used:
 
# A=ALAnine B=GLUtamine?* C=CYSteine D=ASPartate E=GLUtamate
 
# F=PHEnylalanine G=GLYcine H=HIStidine I=IsoLEucine K=LYSine
 
# L=LEUcine M=METhionine N=ASparagiNe O=PYrroLysine*** P=PROline
 
# Q=GLutamiNe R=ARGinine S=SERine T=THReonine U=SElenoCysteine
 
# V=VALine W=TRyPtophan X=UNKnown**** Y=TYRosine Z=ASparagiNe?**
 
#   *Either GLU or GLN: drawn as GLN with chi3 flipped
 
#   **Either ASP or ASN: drawn as ASN with chi3 flipped
 
# ***Not supported
 
# ****Unknown aa will be drawn as ALA
 
#
 
 
 
# The following constant values determine the pitch of the alpha helix
 
var PHI = -50 # Dihedral angle of N-CA bond (nominally -50)
 
var PSI = -60 # Dihedral angle of CA-C bond (nominally -60)
 
var OMEGA = 180 # Dihedral angle of the peptide bond (nominally 180)
 
var PEPTIDE_ANGLE = 110 # C-N-CA angle (nominally 110)
 
var PRO_BUMP = -15 # Psi angle change to N-3psi when N is Pro
 
 
 
# Lookup 3 letter code from 1 letter code
 
function get3from1(c) {
 
ret = ""
 
switch (c) {
 
case 'A':
 
case 'X':
 
ret = "ALA";
 
break;
 
case 'C':
 
ret = "CYS";
 
break;
 
case 'D':
 
ret = "ASP";
 
break;
 
case 'E':
 
ret = "GLU";
 
break;
 
case 'F':
 
ret = "PHE";
 
break;
 
case 'G':
 
ret = "GLY";
 
break;
 
case 'H':
 
ret = "HIS";
 
break;
 
case 'I':
 
ret = "ILE";
 
break;
 
case 'K':
 
ret = "LYS";
 
break;
 
case 'L':
 
ret = "LEU";
 
break;
 
case 'M':
 
ret = "MET";
 
break;
 
case 'N':
 
case 'Z':
 
ret = "ASN";
 
break;
 
case 'P':
 
ret = "PRO";
 
break;
 
case 'B':
 
case 'Q':
 
ret = "GLN";
 
break;
 
case 'R':
 
ret = "ARG";
 
break;
 
case 'S':
 
ret = "SER";
 
break;
 
case 'T':
 
ret = "THR";
 
break;
 
case 'U':
 
ret = "SEC";
 
break;
 
case 'V':
 
ret = "VAL";
 
break;
 
case 'W':
 
ret = "TRP";
 
break;
 
case 'Y':
 
ret = "TYR";
 
break;
 
}
 
return ret
 
};
 
 
 
# Generate PDM atom record
 
function genAtom(n, e, aa, i, xyz) {
 
a =  format("ATOM  %5d  %3s %3s A", n, e, aa )         
 
a +=  format("%4d    %8.3f", i, xyz[1] )         
 
a +=  format("%8.3f%8.3f\n", xyz[2], xyz[3] )
 
return a
 
};
 
 
 
# Generate an amino acid record set
 
function genAA(i, aa, x) {
 
n = x
 
 
 
# From constructed AAs
 
N0 = [0.0, 0.0, 0.0]
 
CA = [ 0.200, 1.174, 0.911 ]
 
C  = [ -1.110, 1.668, 1.425 ] #[ -1.129, 1.783, 1.241 ]
 
O  = [ -1.320, 1.693, 2.62 ] #[ -1.241, 1.967, 2.726 ]
 
CB = [ 1.062, 2.1950, 0.230 ]
 
 
G1 = [ 2.359, 1.607, -0.344] #2.396, 1.588, -0.091 ]
 
G2 = [ 1.363, 3.336, 1.157 ] #0.680, 3.652, 0.423]
 
D1 = [ 3.222, 2.656, -1.048 ] #[ 3.225, 2.340, -1.096]
 
D2 = [ 3.143, 0.904, 0.725 ] #[ 3.189, 1.093, 1.087]
 
E1 = [ 3.645, 3.749, -0.167 ] #[ 3.652, 3.503, -0.111 ]
 
E2 = [ 2.491, 3.234, -2.249 ] #[ 4.342, 1.591, -1.456 ]
 
Z  = [ 4.470, 4.717, -0.885 ] #[ 4.115, 3.339, 1.403 ]
 
H1 = [ 4.450, 6.006, -0.220 ] #[4.087, 4.572, 2.139]
 
H2 = [5.833, 4.228, -0.984 ] #[5.469, 2.866, 1.296]
 
 
Gp = [ 2.008, 1.24, -0.46 ]
 
Dp = [1.022, 0.213, -1.031 ]
 
 
Gfy  = [ 2.368, 1.471, -0.0152 ]
 
D1fy = [ 3.346, 1.524, 0.921 ]
 
D2fy = [ 2.493, 0.516, -1.151 ]
 
E1fy = [ 4.513, 0.615, 0.8244 ]
 
E2fy = [ 3.528, -0.336, -1.206 ]
 
Zfy  = [ 4.588, -0.285, -0.168 ]
 
Hfy = [ 5.738, -1.245, -0.233 ]
 
 
Ghw  = [ 2.406, 1.626, -0.134 ]
 
D1hw = [3.498, 1.936, 0.675]
 
D2hw = [ 2.713, 0.901, -1.211 ]
 
E1hw = [ 4.160, 0.518, -1.178 ]
 
E2hw = [ 4.622, 1.160, 0.0816 ]
 
E3hw = [ 3.789, 2.523, 1.944 ]
 
Z2hw = [ 5.973, 1.177, 0.689 ]
 
Z3hw = [ 5.014, 2.550, 2.503 ]
 
H2hw = [ 6.153, 1.846, 1.844 ]
 
 
N1 = [ 2.069, -2.122, -0.554] #[ -1.965, 2.307, 0.206 ]
 
 
# Build PDB atom records common to all AAs
 
a3 = get3from1(seq[i])
 
if (a3 == "") {
 
a3 = "UNK"
 
}
 
print format("+ %s%d", a3, i)
 
a = genAtom(n++, "N  ", a3, i, N0)
 
a += genAtom(n++, "CA ", a3, i, CA)
 
a += genAtom(n++, "C  ", a3, i, C)
 
a += genAtom(n++, "O  ", a3, i, O)
 
if (seq[i] != 'G') {
 
a += genAtom(n++, "CB ", a3, i, CB)
 
}
 
 
 
# Now add AA specific atom records
 
switch (aa) {
 
case 'A' :
 
case 'X' :
 
break;
 
case 'B' :
 
a += genAtom(n++, "CG ", a3, i, G1)
 
a += genAtom(n++, "CD ", a3, i, D1)
 
a += genAtom(n++, "OE1", a3, i, E2) # GLN with Es switched
 
a += genAtom(n++, "NE2", a3, i, E1)
 
break;
 
case 'C' :
 
a += genAtom(n++, "SG ", a3, i, G2)
 
break;
 
case 'D' :
 
a += genAtom(n++, "CG ", a3, i, G1)
 
a += genAtom(n++, "OD1", a3, i, D1)
 
a += genAtom(n++, "OD2", a3, i, D2)
 
break;
 
case 'E' :
 
a += genAtom(n++, "CG ", a3, i, G1)
 
a += genAtom(n++, "CD ", a3, i, D1)
 
a += genAtom(n++, "OE1", a3, i, E1)
 
a += genAtom(n++, "OE2", a3, i, E2)
 
break;
 
case 'F' :
 
a += genAtom(n++, "CG ", a3, i, Gfy)
 
a += genAtom(n++, "CD1", a3, i, D1fy)
 
a += genAtom(n++, "CD2", a3, i, D2fy)
 
a += genAtom(n++, "CE1", a3, i, E1fy)
 
a += genAtom(n++, "CE2", a3, i, E2fy)
 
a += genAtom(n++, "CZ ", a3, i, Zfy)
 
break;
 
case 'G' :
 
break;
 
case 'H' :
 
a += genAtom(n++, "CG ", a3, i, Ghw)
 
a += genAtom(n++, "ND1", a3, i, D1hw)
 
a += genAtom(n++, "CD2", a3, i, D2hw)
 
a += genAtom(n++, "CE1", a3, i, E2hw)
 
a += genAtom(n++, "NE2", a3, i, E1hw)
 
break;
 
case 'I' :
 
a += genAtom(n++, "CG1", a3, i, G1)
 
a += genAtom(n++, "CG2", a3, i, G2)
 
a += genAtom(n++, "CD1", a3, i, D1)
 
break;
 
case 'K' :
 
a += genAtom(n++, "CG ", a3, i, G1)
 
a += genAtom(n++, "CD ", a3, i, D1)
 
a += genAtom(n++, "CE ", a3, i, E1)
 
a += genAtom(n++, "NZ ", a3, i, Z)
 
break;
 
case 'L' :
 
a += genAtom(n++, "CG1", a3, i, G1)
 
a += genAtom(n++, "CD1", a3, i, D1)
 
a += genAtom(n++, "CD2", a3, i, D2)
 
break;
 
case 'M' :
 
a += genAtom(n++, "CG ", a3, i, G1)
 
a += genAtom(n++, "SD ", a3, i, D1)
 
a += genAtom(n++, "CE ", a3, i, E1)
 
break;
 
case 'N' :
 
a += genAtom(n++, "CG ", a3, i, G1)
 
a += genAtom(n++, "OD1", a3, i, D1)
 
a += genAtom(n++, "ND2", a3, i, D2)
 
break;
 
case 'P' :
 
a += genAtom(n++, "CG ", a3, i, GP)
 
a += genAtom(n++, "CD ", a3, i, DP)
 
break;
 
case 'Q' :
 
a += genAtom(n++, "CG ", a3, i, G1)
 
a += genAtom(n++, "CD ", a3, i, D1)
 
a += genAtom(n++, "OE1", a3, i, E1)
 
a += genAtom(n++, "NE2", a3, i, E2)
 
break;
 
case 'R' :
 
a += genAtom(n++, "CG ", a3, i, G1)
 
a += genAtom(n++, "CD ", a3, i, D1)
 
a += genAtom(n++, "NE ", a3, i, E1)
 
a += genAtom(n++, "CZ ", a3, i, Z)
 
a += genAtom(n++, "NH1", a3, i, H1)
 
a += genAtom(n++, "NH2", a3, i, H2)
 
break;
 
case 'S' :
 
a += genAtom(n++, "OG ", a3, i, G1)
 
break;
 
case 'T' :
 
a += genAtom(n++, "OG1", a3, i, G1)
 
a += genAtom(n++, "CG2", a3, i, G2)
 
break;
 
case 'U' :
 
a += genAtom(n++, "SeG", a3, i, G1)
 
break;
 
case 'V' :
 
a += genAtom(n++, "CG1", a3, i, G1)
 
a += genAtom(n++, "CG2", a3, i, G2)
 
break;
 
case 'W' :
 
a += genAtom(n++, "CG ", a3, i, Ghw)
 
a += genAtom(n++, "CD1", a3, i, D1hw)
 
a += genAtom(n++, "CD2", a3, i, D2hw)
 
a += genAtom(n++, "CE2", a3, i, E2hw)
 
a += genAtom(n++, "NE1", a3, i, E1hw)
 
a += genAtom(n++, "CE3", a3, i, E3hw)
 
a += genAtom(n++, "CZ2", a3, i, Z2hw)
 
a += genAtom(n++, "CZ3", a3, i, Z3hw)
 
a += genAtom(n++, "CH2", a3, i, H2hw)
 
break;
 
case 'Y' :
 
a += genAtom(n++, "CG ", a3, i, Gfy)
 
a += genAtom(n++, "CD1", a3, i, D1fy)
 
a += genAtom(n++, "CD2", a3, i, D2fy)
 
a += genAtom(n++, "CE1", a3, i, E1fy)
 
a += genAtom(n++, "CE2", a3, i, E2fy)
 
a += genAtom(n++, "CZ ", a3, i, Zfy)
 
a += genAtom(n++, "OH ", a3, i, Hfy)
 
break;
 
case 'Z' :
 
a += genAtom(n++, "CG ", a3, i, G1)
 
a += genAtom(n++, "OD1", a3, i, D2) # ASN with Ds switched
 
a += genAtom(n++, "ND2", a3, i, D1)
 
break;
 
default :
 
break;
 
}
 
 
 
return a
 
};
 
 
 
function rotateNward (a1, a2, angle) {
 
select atomno<a1
 
fix atomno>=a2
 
rotateselected {atomno=a1} {atomno=a2} @angle
 
#print format("a1=%d a2=%d angle=%d", a1, a2, angle) #DEBUG
 
 
 
};
 
 
 
# GenAlph
 
function genAlpha(seq, PHI, PSI, OMEGA, PEPTIDE_ANGLE, PRO_BUMP) {
 
 
 
# For each aa
 
set appendnew false
 
n = 1
 
pn = 0
 
pc= 0 # previous C
 
ca1 = 0; ca2 = 0; ca3 = 0
 
for (var i = 1; i <= seq.count; i++) {
 
 
 
# Step previous N
 
pn = n
 
 
 
# Move polypeptide C to bond distance from new AA N
 
select all
 
fix none
 
translateselected {2.069, -2.122, -0.554 } #N1
 
 
 
# Gen AA
 
a = "data \"append aa\"\n"
 
a += genAA(i, seq[i], n);
 
a += "end \"append aa\""
 
script inline @{a}
 
 
 
# If PRO
 
# Adjust i-3psi as rigid PRO D4 bumps Oi-4 as i-3psi
 
# is the most torqued psi and psis are the easiest to twist
 
if (seq[i] == 'P') {
 
rotateNward (ca3, ca3+1, PRO_BUMP)
 
}
 
 
 
# If not first AA
 
if (pc > 0) {
 
 
 
# Gen axis on previous n perpendicular to the plane
 
# containing atoms pc, pn and pn+1
 
v1={atomno=pc}.xyz - {atomno=pn}.xyz
 
v2={atomno=@{pn+1}}.xyz - {atomno=pn}.xyz
 
axis = cross(v1, v2)
 
 
# Center on atom previous n
 
axis += {atomno=pn}.xyz
 
 
 
# Rotate the polypeptide N on the new AA C to the
 
# desired angle (nominally 110)
 
select atomno<pn
 
fix atomno>=pn
 
rotateselected @axis {atomno=pn} @{PEPTIDE_ANGLE - 77}
 
 
 
# Make omega dihedral OMEGA (nominally 180)
 
rotateselected {atomno=pc} {atomno=pn} @{OMEGA - 123}
 
 
 
# Make the phi PHI (nominally -50)
 
rotateselected {atomno=pn} {atomno=@{pn+1}} @{PHI - 30}
 
 
 
# Make the psi PSI (nominally -60)
 
fix atomno>pca
 
select atomno<pn and (atomno != @{pc+1})
 
rotateselected {atomno=pc} {atomno=@{pc-1}} @{PSI + 60}
 
 
 
# If aromatic go trans on chi 1
 
select atomno>@{pn+4} and atomno<n
 
if ((seq[i] == 'H') || (seq[i] == 'W') || (seq[i] == 'F') || (seq[i] == 'Y')) {
 
#rotateselected {atomno=@{pn+1}} {atomno=@{pn+4}} -60
 
}
 
 
 
# Save last three CAs for proline bumps
 
ca3 = ca2; ca2 = ca1; ca1 = pn + 1
 
}
 
 
# Step previous C
 
pc =pn + 2
 
 
 
# Make the peptide bond
 
connect
 
}
 
 
# Clean up
 
select all
 
fix none
 
}
 
 
 
echo Generating Alpha Helix
 
 
 
# Get the sequence from the user
 
seq = prompt("*** Any existing will be cleared ***\nEnter AA sequence (1 char coded)", "")%9999
 
if (seq.count > 0) {
 
zap # disable to keep existing structures
 
print format ("seq=%s  phi=%d  psi=%d", seq, PHI, PSI)
 
print format ("phi=%d  psi=%d  peptide angle=%d  pro bump=%d", PEPTIDE_ANGLE, PRO_BUMP)
 
genAlpha(seq, PHI,PSI, OMEGA, PEPTIDE_ANGLE, PRO_BUMP) # defined at top of scripts
 
}
 
</pre>
 

Latest revision as of 21:32, 31 October 2013

What I had here before belongs on the user page - so I moved it...

Contributors

Remig

Retrieved from "https://wiki.jmol.org/index.php?title=User_talk:Remig&oldid=8180"