pdb2gmx input files¶
The GROMACS program pdb2gmx generates a topology for the input
coordinate file. Several formats are supported for that coordinate file,
but pdb is the most commonly-used format (hence the name pdb2gmx).
pdb2gmx searches for force fields in sub-directories of the GROMACS
share/top
directory and your working directory. Force fields are
recognized from the file forcefield.itp
in a directory with the
extension .ff
. The file forcefield.doc
may be present, and if so, its
first line will be used by pdb2gmx to present a short description to the
user to help in choosing a force field. Otherwise, the user can choose a
force field with the -ff xxx
command-line argument to pdb2gmx, which
indicates that a force field in a xxx.ff
directory is desired. pdb2gmx
will search first in the working directory, then in the GROMACS
share/top
directory, and use the first matching xxx.ff
directory found.
Two general files are read by pdb2gmx: an atom type file (extension
atp, see Atom types) from the force-field directory, and a file
called residuetypes.dat
from either the working directory, or the
GROMACS share/top
directory. residuetypes.dat
determines which residue
names are considered protein, DNA, RNA, water, and ions.
pdb2gmx can read one or multiple databases with topological information for different types of molecules. A set of files belonging to one database should have the same basename, preferably telling something about the type of molecules (e.g. aminoacids, rna, dna). The possible files are:
<basename>.rtp
<basename>.r2b (optional)
<basename>.arn (optional)
<basename>.hdb (optional)
<basename>.n.tdb (optional)
<basename>.c.tdb (optional)
Only the rtp file, which contains the topologies of the building
blocks, is mandatory. Information from other files will only be used for
building blocks that come from an rtp file with the same base name. The
user can add building blocks to a force field by having additional files
with the same base name in their working directory. By default, only
extra building blocks can be defined, but calling pdb2gmx with the -rtpo
option will allow building blocks in a local file to replace the default
ones in the force field.
Residue database¶
The files holding the residue databases have the extension rtp.
Originally this file contained building blocks (amino acids) for
proteins, and is the GROMACS interpretation of the rt37c4.dat
file of
GROMOS. So the residue database file contains information (bonds,
charges, charge groups, and improper dihedrals) for a frequently-used
building block. It is better not to change this file because it is
standard input for pdb2gmx, but if changes are needed make them in the
top file (see Topology file), or in a rtp file in the working
directory as explained in sec. pdb2gmx input files. Defining topologies
of new small molecules is probably easier by writing an include topology
file itp directly. This will be discussed in section Molecule.itp file.
When adding a new protein residue to the database, don’t forget to add
the residue name to the residuetypes.dat file, so that grompp, make_ndx
and analysis tools can recognize the residue as a protein residue (see
Default Groups).
The rtp files are only used by pdb2gmx. As mentioned before, the only extra information this program needs from the rtp database is bonds, charges of atoms, charge groups, and improper dihedrals, because the rest is read from the coordinate input file. Some proteins contain residues that are not standard, but are listed in the coordinate file. You have to construct a building block for this “strange” residue, otherwise you will not obtain a top file. This also holds for molecules in the coordinate file such as ligands, polyatomic ions, crystallization co-solvents, etc. The residue database is constructed in the following way:
[ bondedtypes ] ; mandatory
; bonds angles dihedrals impropers
1 1 1 2 ; mandatory
[ GLY ] ; mandatory
[ atoms ] ; mandatory
; name type charge chargegroup
N N -0.280 0
H H 0.280 0
CA CH2 0.000 1
C C 0.380 2
O O -0.380 2
[ bonds ] ; optional
;atom1 atom2 b0 kb
N H
N CA
CA C
C O
-C N
[ exclusions ] ; optional
;atom1 atom2
[ angles ] ; optional
;atom1 atom2 atom3 th0 cth
[ dihedrals ] ; optional
;atom1 atom2 atom3 atom4 phi0 cp mult
[ impropers ] ; optional
;atom1 atom2 atom3 atom4 q0 cq
N -C CA H
-C -CA N -O
[ ZN ]
[ atoms ]
ZN ZN 2.000 0
The file is free format; the only restriction is that there can be at
most one entry on a line. The first field in the file is the [ bondedtypes ]
field,
which is followed by four numbers, indicating the interaction type for
bonds, angles, dihedrals, and improper dihedrals. The file contains
residue entries, which consist of atoms and (optionally) bonds, angles,
dihedrals, and impropers. The charge group codes denote the charge group
numbers. Atoms in the same charge group should always be ordered
consecutively. When using the hydrogen database with pdb2gmx for adding
missing hydrogens (see hdb), the atom names defined in the rtp
entry should correspond exactly to the naming convention used in the
hydrogen database. The atom names in the bonded interaction can be
preceded by a minus or a plus, indicating that the atom is in the
preceding or following residue respectively. Explicit parameters added
to bonds, angles, dihedrals, and impropers override the standard
parameters in the itp files. This should only be used in special cases.
Instead of parameters, a string can be added for each bonded
interaction. This is used in GROMOS-96 rtp files. These strings are
copied to the topology file and can be replaced by force-field
parameters by the C-preprocessor in grompp using #define
statements.
pdb2gmx automatically generates all angles. This means
that for most force fields the [ angles ]
field is only
useful for overriding itp parameters. For the GROMOS-96
force field the interaction number of all angles needs to be specified.
pdb2gmx automatically generates one proper dihedral for every rotatable
bond, preferably on heavy atoms. When the [ dihedrals ]
field is used, no other
dihedrals will be generated for the bonds corresponding to the specified
dihedrals. It is possible to put more than one dihedral function on a
rotatable bond. In the case of CHARMM27 FF pdb2gmx can add correction
maps to the dihedrals using the default -cmap
option. Please refer to
CHARMM for more information.
pdb2gmx sets the number of exclusions to 3, which means
that interactions between atoms connected by at most 3 bonds are
excluded. Pair interactions are generated for all pairs of atoms that
are separated by 3 bonds (except pairs of hydrogens). When more
interactions need to be excluded, or some pair interactions should not
be generated, an [ exclusions ]
field can be added,
followed by pairs of atom names on separate lines. All non-bonded and
pair interactions between these atoms will be excluded.
Residue to building block database¶
Each force field has its own naming convention for residues. Most residues have consistent naming, but some, especially those with different protonation states, can have many different names. The r2b files are used to convert standard residue names to the force-field build block names. If no r2b is present in the force-field directory or a residue is not listed, the building block name is assumed to be identical to the residue name. The r2b can contain 2 or 5 columns. The 2-column format has the residue name in the first column and the building block name in the second. The 5-column format has 3 additional columns with the building block for the residue occurring in the N-terminus, C-terminus and both termini at the same time (single residue molecule). This is useful for, for instance, the AMBER force fields. If one or more of the terminal versions are not present, a dash should be entered in the corresponding column.
There is a GROMACS naming convention for residues which is only apparent
(except for the pdb2gmx code) through the
r2b file and specbond.dat
files. This
convention is only of importance when you are adding residue types to an
rtp file. The convention is listed in Table 12.
For special bonds with, for instance,
a heme group, the GROMACS naming convention is introduced through
specbond.dat
(see Special bonds),
which can subsequently be translated by the r2b file,
if required.
GROMACS ID | Residue | |
---|---|---|
ARG | protonated arginine | |
ARGN | neutral arginine | |
ASP | negatively charged aspartic acid | |
ASPH | neutral aspartic acid | |
CYS | neutral cysteine | |
CYS2 | cysteine with sulfur bound to another cysteine or a heme | |
GLU | negatively charged glutamic acid | |
GLUH | neutral glutamic acid | |
HISD | neutral histidine with N\(_\delta\) protonated | |
HISE | neutral histidine with N\(_\epsilon\) protonated | |
HISH | positive histidine with both N\(_\delta\) and N\(_\epsilon\) protonated | |
HIS1 | histidine bound to a heme | |
LYSN | neutral lysine | |
LYS | protonated lysine | |
HEME | heme |
Atom renaming database¶
Force fields often use atom names that do not follow IUPAC or PDB convention. The arn database is used to translate the atom names in the coordinate file to the force-field names. Atoms that are not listed keep their names. The file has three columns: the building block name, the old atom name, and the new atom name, respectively. The residue name supports question-mark wildcards that match a single character.
An additional general atom renaming file called
xlateat.dat
is present in the share/top
directory, which translates common non-standard atom names in the
coordinate file to IUPAC/PDB convention. Thus, when writing force-field
files, you can assume standard atom names and no further atom name
translation is required, except for translating from standard atom names
to the force-field ones.
Hydrogen database¶
The hydrogen database is stored in hdb files. It contains information
for the pdb2gmx program on how to connect hydrogen atoms to existing
atoms. In versions of the database before GROMACS 3.3, hydrogen atoms
were named after the atom they are connected to: the first letter of the
atom name was replaced by an ‘H.’ In the versions from 3.3 onwards, the
H atom has to be listed explicitly, because the old behavior was
protein-specific and hence could not be generalized to other molecules.
If more than one hydrogen atom is connected to the same atom, a number
will be added to the end of the hydrogen atom name. For example, adding
two hydrogen atoms to ND2
(in asparagine), the hydrogen atoms will
be named HD21
and HD22
. This is important since atom naming in
the rtp file (see rtp) must be the same. The format of the
hydrogen database is as follows:
; res # additions
# H add type H i j k
ALA 1
1 1 H N -C CA
ARG 4
1 2 H N CA C
1 1 HE NE CD CZ
2 3 HH1 NH1 CZ NE
2 3 HH2 NH2 CZ NE
On the first line we see the residue name (ALA or ARG) and the number of kinds of hydrogen atoms that may be added to this residue by the hydrogen database. After that follows one line for each addition, on which we see:
The number of H atoms added
The method for adding H atoms, which can be any of:
- one planar hydrogen, e.g. rings or peptide bondOne hydrogen atom (n) is generated, lying in the plane of atoms (i,j,k) on the plane bisecting angle (j-i-k) at a distance of 0.1 nm from atom i, such that the angles (n-i-j) and (n-i-k) are \(>\) 90\(^{\rm o}\).
- one single hydrogen, e.g. hydroxylOne hydrogen atom (n) is generated at a distance of 0.1 nm from atom i, such that angle (n-i-j)=109.5 degrees and dihedral (n-i-j-k)=trans.
- two planar hydrogens, e.g. ethylene -C=CH\(_2\), or amide -C(=O)NH\(_2\)Two hydrogens (n1,n2) are generated at a distance of 0.1 nm from atom i, such that angle (n1-i-j)=(n2-i-j)=120 degrees and dihedral (n1-i-j-k)=cis and (n2-i-j-k)=trans, such that names are according to IUPAC standards 129.
- two or three tetrahedral hydrogens, e.g. -CH\(_3\)Three (n1,n2,n3) or two (n1,n2) hydrogens are generated at a distance of 0.1 nm from atom i, such that angle (n1-i-j)=(n2-i-j)=(n3-i-j)=109.47:math:^{rm o}, dihedral (n1-i-j-k)=trans, (n2-i-j-k)=trans+120 and (n3-i-j-k)=trans+240:math:^{rm o}.
- one tetrahedral hydrogen, e.g. C\(_3\)* CH*One hydrogen atom (n:math:^prime) is generated at a distance of 0.1 nm from atom i in tetrahedral conformation such that angle (n:math:^prime-i-j)=(n:math:^prime-i-k)=(n:math:^prime-i-l)=109.47:math:^{rm o}.
- two tetrahedral hydrogens, e.g. C-CH\(_2\)*-C*Two hydrogen atoms (n1,n2) are generated at a distance of 0.1 nm from atom i in tetrahedral conformation on the plane bisecting angle j-i-k with angle (n1-i-n2)=(n1-i-j)=(n1-i-k)=109.47:math:^{rm o}.
- two water hydrogensTwo hydrogens are generated around atom i according to SPC 80 water geometry. The symmetry axis will alternate between three coordinate axes in both directions.
- three water “hydrogens”Two hydrogens are generated around atom i according to SPC 80 water geometry. The symmetry axis will alternate between three coordinate axes in both directions. In addition, an extra particle is generated on the position of the oxygen with the first letter of the name replaced by ‘M’. This is for use with four-atom water models such as TIP4P 128.
- four water “hydrogens”Same as above, except that two additional particles are generated on the position of the oxygen, with names ‘LP1’ and ‘LP2.’ This is for use with five-atom water models such as TIP5P 130.
The name of the new H atom (or its prefix, e.g.
HD2
for the asparagine example given earlier).Three or four control atoms (i,j,k,l), where the first always is the atom to which the H atoms are connected. The other two or three depend on the code selected. For water, there is only one control atom.
Some more exotic cases can be approximately constructed from the above tools, and with suitable use of energy minimization are good enough for beginning MD simulations. For example secondary amine hydrogen, nitrenyl hydrogen (\(\mathrm{C}=\mathrm{NH}\)) and even ethynyl hydrogen could be approximately constructed using method 2 above for hydroxyl hydrogen.
Termini database¶
The termini
databases
are stored in aminoacids.n.tdb
and
aminoacids.c.tdb
for the N- and C-termini respectively.
They contain information for the pdb2gmx program on how
to connect new atoms to existing ones, which atoms should be removed or
changed, and which bonded interactions should be added. Their format is
as follows (from gromos43a1.ff/aminoacids.c.tdb
):
[ None ]
[ COO- ]
[ replace ]
C C C 12.011 0.27
O O1 OM 15.9994 -0.635
OXT O2 OM 15.9994 -0.635
[ add ]
2 8 O C CA N
OM 15.9994 -0.635
[ bonds ]
C O1 gb_5
C O2 gb_5
[ angles ]
O1 C O2 ga_37
CA C O1 ga_21
CA C O2 ga_21
[ dihedrals ]
N CA C O2 gd_20
[ impropers ]
C CA O2 O1 gi_1
The file is organized in blocks, each with a header specifying the name
of the block. These blocks correspond to different types of termini that
can be added to a molecule. In this example [ COO- ]
is
the first block, corresponding to changing the terminal carbon atom into
a deprotonated carboxyl group. [ None ]
is the second
terminus type, corresponding to a terminus that leaves the molecule as
it is. Block names cannot be any of the following:
replace
, add
, delete
,
bonds
, angles
,
dihedrals
, impropers
. Doing so would
interfere with the parameters of the block, and would probably also be
very confusing to human readers.
For each block the following options are present:
[ replace ]
Replace an existing atom by one with a different atom type, atom name, charge, and/or mass. This entry can be used to replace an atom that is present both in the input coordinates and in the rtp database, but also to only rename an atom in the input coordinates such that it matches the name in the force field. In the latter case, there should also be a corresponding[ add ]
section present that gives instructions to add the same atom, such that the position in the sequence and the bonding is known. Such an atom can be present in the input coordinates and kept, or not present and constructed by pdb2gmx. For each atom to be replaced on line should be entered with the following fields:- name of the atom to be replaced
- new atom name (optional)
- new atom type
- new mass
- new charge
[ add ]
Add new atoms. For each (group of) added atom(s), a two-line entry is necessary. The first line contains the same fields as an entry in the hydrogen database (name of the new atom, number of atoms, type of addition, control atoms, see hdb), but the possible types of addition are extended by two more, specifically for C-terminal additions:- two carboxyl oxygens, -COO\(^-\)Two oxygens (n1,n2) are generated according to rule 3, at a distance of 0.136 nm from atom i and an angle (n1-i-j)=(n2-i-j)=117 degrees
- carboxyl oxygens and hydrogen, -COOHTwo oxygens (n1,n2) are generated according to rule 3, at distances of 0.123 nm and 0.125 nm from atom i for n1 and n2, respectively, and angles (n1-i-j)=121 and (n2-i-j)=115 degrees. One hydrogen (n:math:^prime) is generated around n2 according to rule 2, where n-i-j and n-i-j-k should be read as n\(^\prime\)-n2-i and n\(^\prime\)-n2-i-j, respectively.
After this line, another line follows that specifies the details of the added atom(s), in the same way as for replacing atoms, i.e.:
- atom type
- mass
- charge
- charge group (optional)
Like in the hydrogen database (see rtp), when more than one atom is connected to an existing one, a number will be appended to the end of the atom name. Note that, like in the hydrogen database, the atom name is now on the same line as the control atoms, whereas it was at the beginning of the second line prior to GROMACS version 3.3. When the charge group field is left out, the added atom will have the same charge group number as the atom that it is bonded to.
[ delete ]
Delete existing atoms. One atom name per line.
Virtual site database¶
Since we cannot rely on the positions of hydrogens in input files, we need a special input file to decide the geometries and parameters with which to add virtual site hydrogens. For more complex virtual site constructs (e.g. when entire aromatic side chains are made rigid) we also need information about the equilibrium bond lengths and angles for all atoms in the side chain. This information is specified in the vsd file for each force field. Just as for the termini, there is one such file for each class of residues in the rtp file.
The virtual site database is not really a very simple list of
information. The first couple of sections specify which mass centers
(typically called MCH\(_3\)/MNH:math:_3) to use for
CH\(_3\), NH\(_3\), and NH\(_2\) groups. Depending on
the equilibrium bond lengths and angles between the hydrogens and heavy
atoms we need to apply slightly different constraint distances between
these mass centers. Note that we do not have to specify the actual
parameters (that is automatic), just the type of mass center to use. To
accomplish this, there are three sections names [ CH3 ]
,
[ NH3 ]
, and [ NH2 ]
. For each of these we expect three columns.
The first column is the atom type bound to the 2/3 hydrogens, the second
column is the next heavy atom type which this is bound, and the third
column the type of mass center to use. As a special case, in the
[ NH2 ]
section it is also possible to specify planar
in the
second column, which will use a different construction without mass
center. There are currently different opinions in some force fields
whether an NH\(_2\) group should be planar or not, but we try hard
to stick to the default equilibrium parameters of the force field.
The second part of the virtual site database contains explicit
equilibrium bond lengths and angles for pairs/triplets of atoms in
aromatic side chains. These entries are currently read by specific
routines in the virtual site generation code, so if you would like to
extend it e.g. to nucleic acids you would also need to write new code
there. These sections are named after the short amino acid names
([ PHE ]
, [ TYR ]
, [ TRP ]
, [ HID ]
, [ HIE ]
,
[ HIP ]
), and simply contain 2 or 3 columns with atom names,
followed by a number specifying the bond length (in nm) or angle (in
degrees). Note that these are approximations of the equilibrated
geometry for the entire molecule, which might not be identical to the
equilibrium value for a single bond/angle if the molecule is strained.
Special bonds¶
The primary mechanism used by
pdb2gmx to generate
inter-residue bonds relies on head-to-tail linking of backbone atoms in
different residues to build a macromolecule. In some cases (e.g.
disulfide bonds, a heme
group, branched
polymers), it is necessary to
create inter-residue bonds that do not lie on the backbone. The file
specbond.dat
takes
care of this function. It is necessary that the residues belong to the
same [ moleculetype ]
. The -merge
and
-chainsep
functions of pdb2gmx can be
useful when managing special inter-residue bonds between different
chains.
The first line of specbond.dat
indicates the number of
entries that are in the file. If you add a new entry, be sure to
increment this number. The remaining lines in the file provide the
specifications for creating bonds. The format of the lines is as
follows:
resA atomA nbondsA resB atomB nbondsB length newresA
newresB
The columns indicate:
resA
The name of residue A that participates in the bond.atomA
The name of the atom in residue A that forms the bond.nbondsA
The total number of bondsatomA
can form.resB
The name of residue B that participates in the bond.atomB
The name of the atom in residue B that forms the bond.nbondsB
The total number of bondsatomB
can form.length
The reference length for the bond. IfatomA
andatomB
are not withinlength
\(\pm\) 10% in the coordinate file supplied to pdb2gmx, no bond will be formed.newresA
The new name of residue A, if necessary. Some force fields use e.g. CYS2 for a cysteine in a disulfide or heme linkage.newresB
The new name of residue B, likewise.