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> Please Let me ask two more simple questions about solv
- Original Message -
From: jojo J
Date: Thursday, July 8, 2010 13:17
Subject: [gmx-users] energy contributions / question about solvating
To: gmx-users@gromacs.org
> Hello everyone,
>
> I have a question on LJ and coulomb 1-4 energy terms. These are considered as
> intramolecular inte
Hello everyone,
I have a question on LJ and coulomb 1-4 energy terms. These are considered
as intramolecular interactions and LJ and coulomb SR as intermolecular. If
nrexcl in top file is 3, this means we obtain 1-4 energies, 1-5, 1-6,
Now what we calculate as intermolecular (SR) contributions
Sai Pooja wrote:
Hi Justin,
I do not have the problem of extra hydrogens or a net charge on the NAC
group.
The net charge is not on NAC, it's on the entire peptide. If you're not seeing
it, that makes the bug even more troubling, since it's sporadic. Are you using
the latest git versi
- Original Message -
From: "C. Batistakis"
Date: Wednesday, July 7, 2010 23:19
Subject: [gmx-users] Nitrile_Butadiene_Rubber simulation using Gromos96
To: gromacs
---
| - - - > Dear all
> I am trying to simulate Nitri
- Original Message -
From: nanogroup
Date: Wednesday, July 7, 2010 21:51
Subject: [gmx-users] No such moleculetype SOL
To: gmx-users@gromacs.org
Cc: mark.abra...@anu.edu.au
---
| > Dear Mark, > > Many thanks for your e-mail. >
As a follow-up, it appears that there are several problems with the CHARMM
implementation. I will file a bugzilla with a few other things I found. There
are a number of errors in the aminoacids.rtp file that cause problems. Most of
all, I can't even get pdb2gmx to generate a CHARMM topology
Sai Pooja wrote:
This probably is my ignorance but the error and the "bug" goes when I
replaced CBX with NAC everywhere.
I would suggest filing a bugzilla. I was able to reproduce your problem. If
nothing else, pdb2gmx should not be name-specific. Something very weird is
going on. Mo
Hi
I m trying to compile the gmx development version (from git) on MacOX (Darwin
kernel)
The configure is successful but after I enter make and after lots of output I
get the following:
ld: warning: in /opt/local/lib/libxml2.a, file was built for unsupported file
format which is not the arch
This probably is my ignorance but the error and the "bug" goes when I
replaced CBX with NAC everywhere.
On Wed, Jul 7, 2010 at 4:47 PM, Justin A. Lemkul wrote:
>
>
> Sai Pooja wrote:
>
>> I checked again and the error does not go. Please read the steps below.
>>
>> The pdb file I started off wit
Sai Pooja wrote:
I checked again and the error does not go. Please read the steps below.
The pdb file I started off with did not have any hydrogens. However, the
way I had specified the capping residues in the .rtp file (SEE MARK'S
MAIL), I had to specify hydrogens in the pdb file for the ca
I checked again and the error does not go. Please read the steps below.
The pdb file I started off with did not have any hydrogens. However, the way
I had specified the capping residues in the .rtp file (SEE MARK'S MAIL), I
had to specify hydrogens in the pdb file for the capping residues. So I us
Hi,
The parameters for ATP (and several other building blocks and
molecules) in the GROMOS 53a5 and 53a6 force fields are, AFAIK,
inherited from the older versions, albeit with some modifications to
bring them in line with the rest of the force field. So they weren't
reparameterized and thus do no
I don't have the parameters. You could possibly fudge it by
extrapolating out from SER->CYS->Se_CYS based scaled by
electronegativities of O,S,Se. I'm not saying that this is rigorous,
just that its possible to do. My main point here, though, is to ask if
you *really* need to bother with th
Dear all,
In an attempt to speed up things, I tried to calculate an hessian matrix in
parallel, using two processors and it finished in about half the time when
compared to a single-node run. However, the parallel run produces an .mtx
file that has about half the size of the one obtained in the
Em 7 de julho de 2010 11:47, Luis Paulo escreveu:
> Please
>
> Someone know Gromos parameters for selenium. WE need to simulate the
> Thioredoxin and we need to simulate a cisteine with a selenium.
>
> Thanks
> regards
>
> Luis Scott
>
> --
> Prof. Dr. Luis Paulo Scott
> CMCC- Centro de Matemáti
munu...@yahoo.com wrote:
Hi,
I am using GROMACS 4.0 for simulating a peptide having 5 residues. I
have built the sequence using pymol and capped the peptide with CH3CO
and NHCH3 at its N and C terminal respectively and save in pdb file
format. The pdb file was used to produce *.gro and *.t
I missed that pull_start = yes, sorry. So Gavin, your run should have
stayed around the starting position. Make the histogram directly and
you should get a better idea.
Chris.
-- original message --
To clarify, the tutorial sets "pull_init1 = 0" because it is used in
conjunction
with "p
Hi,
I am using GROMACS 4.0 for simulating a peptide having 5 residues. I have
built the sequence using pymol and capped the peptide with CH3CO and NHCH3 at
its N and C terminal respectively and save in pdb file format. The pdb file
was used to produce *.gro and *.top files using pdb2gmx ff G43
"It seems that I do not need to care about decimal total group charges
as I am planning to use PME."
-- well, find it in the literature first!
-- original message --
Dear Chris,
I really appreciate your comment.
Can you provide a reference for the idea that the charge groups must
have inte
Dear Chris,
I really appreciate your comment.
> Can you provide a reference for the idea that the charge groups must have
> integer charge?
I actually do not have any critical literature for the idea of “whole number
rule”;
1) In the item of “Charge group” of the “GROMACS USER MANUAL, ver.4” i
Gavin Melaugh wrote:
Hi Chris
Thanks very much for your help. The reason I used pull_init1 = 0 is
because this is the value that is used in the tutorial. Maybe I am
misinterpreting its meaning. In the tutorial it says that you do not
have to specify a value separately for each configuration. I
Gavin,
I think it's time for you to read some papers and read the gromacs
manual pull COM section. A few days of reading will make all of this
clear to you.
-- original message --
Hi Chris
Thanks very much for your help. The reason I used pull_init1 = 0 is
because this is the value that i
Hi Chris
Thanks very much for your help. The reason I used pull_init1 = 0 is
because this is the value that is used in the tutorial. Maybe I am
misinterpreting its meaning. In the tutorial it says that you do not
have to specify a value separately for each configuration. I am now
thinking that in
Gavin, let's take g_wham out of the picture for now to simplify
things. First, you umbrella is pretty strange. You want them to have a
distance of 0.0 nm (pull_init1 = 0)???
So let's look at making a histogram from your raw data.
1. cat pullx.xvg |awk '{print sqrt($1,$5*$5+$6*$6+$7*$7)}' > m
perhaps that's not standard terminology, sorry. The numbering starts
at the headgroup so the distal atom would be the one at the end of the
acyl-chain (the one most likely to spend its time in the middle of the
cluster.
-- original message --
Thanks. Just wondering what is a 'distal atom'
Hi Chris
Sorry I sent my e-mail just prior to receiving yours? Is it any clearer?
Gavin
chris.ne...@utoronto.ca wrote:
> The pullx file should contain everything that you need. dX,dY,dZ *are*
> the components of the distances between the two groups.
>
> I still don't understand your question (per
Thanks. Just wondering what is a 'distal atom' as you mentioned.
I am creating a new subject on g_clustsize.
--- On Wed, 7/7/10, chris.ne...@utoronto.ca wrote:
From: chris.ne...@utoronto.ca
Subject: [gmx-users] problem with trjconv -pbc cluster
To: gmx-users@gromacs.org
Date: Wednesday, 7 Ju
Hi Guys
I am having great difficulty generating a histogram of the correct shape
from g_wham. I am running umbrella sampling on one configuration fo two
molecules at a fixed distance using the following
pull parameters. ( I am just running one configuration to begin with so
that can make sure that
The pullx file should contain everything that you need. dX,dY,dZ *are*
the components of the distances between the two groups.
I still don't understand your question (perhaps you could give us a
worked example with real data?), but if you just want the COM
distance, then try this:
cat pul
Nilesh Dhumal wrote:
Hello,
I am trying to equilibrate my system, ionic liquids. Simulations stops
with following error
Fatal error:
1 of the 43778 bonded interactions could not be calculated because some
atoms involved moved further apart than the multi-body cut-off distance
(1.32754 nm) or
Hello,
I am trying to equilibrate my system, ionic liquids. Simulations stops
with following error
Fatal error:
1 of the 43778 bonded interactions could not be calculated because some
atoms involved moved further apart than the multi-body cut-off distance
(1.32754 nm) or the two-body cut-off dist
I wrote my own program to do this and so I never tried that one. We
did find that clustering based on a dingle atom in the chain was a
very good idea. So take your distal carbon in the surfactant and make
in index group of it and cluster it (with a larger cutoff) with
g_clustsize.
Obvious
That depends. mdrun pull code does it smartly via pull_pbcatom
(assuming that you have chosen pull_pbcatom and your box size
smartly), while g_dist is not smart about it at all. Can you be more
specific about what you want to do?
-- original message --
Hi everyone:
How gromacs calculate c
Hi Chris, Thanks a lot for your responses. I will surely try them. But, before
I go to trjconv -pbc cluster, I had one more problem to sort out. This has to
do with quantifying the cluster-size distribution from the trajectory. As I
mentioned, if I visualize the trajectory in VMD, I see that st
Dear Shuntaro:
If you're using PME then there is no need to have unit charge in
charge groups. I can't comment on any other errors that may or may not
be in that topology as I have never simulated ATP. Also, if you're not
using PME, then I can not advise you if it is ok to have non-integer
Dear gmxusers,
I am going to carry out an MD simulation using G53a6 FF, whose system contains
some ATP molecules. In order to know whether the calculation is possible or
not, I looked for a topology of ATP in ffG53a6.rtp. Although the topology
exists, each total charge of charge group 9, 10 a
Dear shuai shuai:
Please use a descriptive title. I renamed it.
You must describe your problem more. e.g. is the problem that you get
a frozen cluster in some simulations, or that you don't get this in
other simulations? What, exactly, is a small cluster of frozen
molecules?
You must als
Dear all,
Recently I met a strong error from gromacs. Therefore I would like to know
whether you have experienced the same thing or what is the reason for that.
The system I simulated is nvt MD for N2 (with partial charge) diffusion in a
long tube (100x2.5x2.5 nm^3) at 300k. The problem is that o
PS:
you realize that trjconv -pbc cluster is never going to work unless
you actually have a cluster, right? So you can't start this procedure
near your initial dispersed state. You need to start at some time T
where you actually do have a cluster. Then you can try -dump T, -dump
(T+X), -d
Dear Jagannath:
There is, as far as I know, no way to fix this. Here's what you should do.
1. Let the space between your timesteps be X ps.
2. Use trjconv -pbc cluster -dump X -o out.gro
2b. if that doesn't work, try trjconv -pbc cluster -dump (X*2) -o out.gro
2c. if that doesn't work, try trjco
Hi everyone:
How gromacs calculate center of mass for broken molecules? If the molecule
is broken due to the pbc, where will the center of mass be?
Thanks,
Kun
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gmx-users mailing listgmx-users@gromacs.org
http://lists.gromacs.org/mailman/listinfo/gmx-users
Please search the archive at http
Dear all
I am trying to simulate
Nitrile-Butadiene-Rubber, using the Gromos96 force field.
I have difficulties in finding the
correct parameters from the bon.itp file , in order to define the polymer in
the .rtp file.
Can someone suggest which parameters
I shall choose in the followin
Hi all
In hindsight I think the question I posted yesterday may have been a
little naive. To rephrase it - If the pullx.xvg files contain X Y Z dX
dY dZ, (because pull_dim = Y Y Y), does the g_wham programme calculate
the centre of mass distances to use in the histogram i.e. Will the first
column
nanogroup wrote:
Dear Mark,
Many thanks for your e-mail.
I checked the TOP file, the SOL is diefined there and numbers of solvent
moelcules are presented.
If this were true, you wouldn't have gotten the error you did. The best
information you can provide is the relevant section of .t
Dear Mark,
Many thanks for your e-mail.
I checked the TOP file, the SOL is diefined there and numbers of solvent
moelcules are presented.
I solved the sample by genbox command and selected spc216.gro
I am looking forward to reading from you.
Bests,
Mahmoud
--
gmx-users mailing l
Hi,
you probably did the covariance analysis on the backbone atoms of your system.
However, for the calculation of the secondary structure PyMOL needs at least
the MainChain part of your molecule. So the easiest thing would be repeat your
analysis with the MainChain group instead of backone.
- Original Message -
From: nanogroup
Date: Wednesday, July 7, 2010 18:16
Subject: [gmx-users] No such moleculetype SOL
To: gmx-users-requ...@gromacs.org
Cc: gmx-users@gromacs.org
---
| > Dear GMX Users,
>
> I solve sample in the w
Hi everyone,
I did a covariance analysis by following this link:
http://nmr.chem.uu.nl/~tsjerk/course/molmod/analysis1.html
Now I want to visualize the differences between the extreme structures by
doing this:
pymol ev?.pdb
Split the models in the pdb files and delete the originals.
split_state
Dear GMX Users,
I solve sample in the water, but when I run GROMPP, this error appeares:
Fatal error:
No such moleculetype SOL
Without water, the grompp was done.
Thanks.
--
gmx-users mailing listgmx-users@gromacs.org
http://lists.gromacs.org/mailman/listinfo/gmx-users
Please sear
Thanks for the reply. I used following command to extract first frame that has
all the surfectants ( as suggested by first step for characterizing micelle
clustering).
trjconv -f a.xtc -o a_cluster.gro -dump 0 -pbc cluster Here is the output I
got:COM: 0.000 0.000 19.999 iter = 195
Dear All,
I am pleased to announce the release of the program RESP ESP charge
Derive version III.4 (or R.E.D. III.4) and its related tools
(Ante_R.E.D.-1.4 and X R.E.D. III.4) available @
http://q4md-forcefieldtools.org/RED/.
New features available:
- Bug corrections and code cleaning in
- Original Message -
From: Kwee Hong
Date: Wednesday, July 7, 2010 11:36
Subject: [gmx-users] problem while simulating metal ions
To: gmx-users@gromacs.org
---
|
>
> Hi.
>
> I'm trying to subject a metalloprotein bound to cad
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