On Tue, 2006-06-20 at 11:31 +1000, Mark Abraham wrote:
> [EMAIL PROTECTED] wrote:
> >
> > Someone has written a script to calculate how may times H2O molecules
> > get really close or bind to the N-terminals of a protein?(it's outer
> > part, not the core) Or maybe someone nows how to calculate
Yes, I did a detailed search about it. The confusing part is nobody complained
about using dummy atoms. Am I missing something?
thanks.
From: "David Mobley" <[EMAIL PROTECTED]>
I think I've seen this one in the archives before. Did you try
searching the list?
On 6/19/06, MURAT CETINKAYA <[EMAIL
Dongsheng Zhang wrote:
Dear David,
yes. I have try it. Even I try to give two different name for two tpr
file, then COPY them to those directories. Both tpr files in one
directory works fine, In the other directory none works.
OK, so speaking in an analogy, here we've told the car mechanic ov
Justin M. Shorb wrote:
Greetings!
I am looking to extract the electrostatic force (non-LJ forces) from an
energy monitoring group. Unfortunately, trying to dig into Gromacs
source without a map is proving to be quite difficult. Can anyone point
me in the direction of the subroutines that hand
[EMAIL PROTECTED] wrote:
Someone has written a script to calculate how may times H2O molecules
get really close or bind to the N-terminals of a protein?(it's outer
part, not the core) Or maybe someone nows how to calculate the N-terms
interactions with the solvent? Anything related to this wou
Sunjoo, is there a particular reason why you want to you anisotropic
pressure coupling? (I recently tried this myself, on a DMPC bilayer).
Some of the key membrane physical properties (like thickness, area per
lipid, order parameters) were distorted and did not agree with
experimental evidence.
Dear Gromacs people
I am trying to run NPT simulation on a bilayer and want to know right setup
to use anisotropic pressure coupling.
I have seen two different cases of reference pressure.
Some people use 1 atm for off-diagonals (xy, yz, zx directions) but other
use 0 atm.
From Erik's answer
Someone has written a script to calculate how may times H2O molecules
get really close or bind to the N-terminals of a protein?(it's outer
part, not the core) Or maybe someone nows how to calculate the N-terms
interactions with the solvent? Anything related to this would help.
__
Hello, in the GMX manual, on page 117, it states:
afm rate1 =
afm rate2 =
The rate at which the spring moves in *nm/ps* for each group.
In my ppa file, I specify:
* afm rate1 = 1*
But in the log file of my mdrun, it states:
Pull rate: 1.00e+00 *nm/ns*. Force constant: 1.00e+03 k
Greetings!
I am looking to extract the electrostatic force (non-LJ forces) from an energy monitoring group. Unfortunately, trying to dig into Gromacs source without a map is proving to be quite difficult. Can anyone point me in the direction of the subroutines that handle:
- output of the forces
Dear David,
yes. I have try it. Even I try to give two different name for two tpr
file, then COPY them to those directories. Both tpr files in one
directory works fine, In the other directory none works.
Dongsheng
On Mon, 2006-06-19 at 13:39 -0700, David Mobley wrote:
> Maybe they're not exa
Maybe they're not exactly identical? Did you try gmxdump and then diff
the output?
David
On 6/19/06, Dongsheng Zhang <[EMAIL PROTECTED]> wrote:
Dear GMX users,
I have two EXACTLY identical tpr files at two different directories on
the SAME machine. When I try to use these two tpr files. One wo
Dear GMX users,
I have two EXACTLY identical tpr files at two different directories on
the SAME machine. When I try to use these two tpr files. One works fine.
Another one gives me bad result, the molecule explodes. Could anyone
tell me why this happens? Thank you in advance!
Dongsheng
On Mon,
I think I've seen this one in the archives before. Did you try
searching the list?
On 6/19/06, MURAT CETINKAYA <[EMAIL PROTECTED]> wrote:
Hi GMX users,
My question is to calculate solvation free energy of a non-standard residue (I
managed to define it into oplsaa database). I followed the tutor
Jianwei Wang wrote:
Hello, I got an error message while using 8 processors becuase of Shake
block crossing node boundaries. Everything was fine when I used a single
processor. Any idea how to ease this problem? Thanks! JW
use max 3 or 4 processors
The error message:
splitting to
Dear GMX users,
I am studying the interaction between a polymer chain and a nanotube in
vacuum. After I set up my system, I use vmd to visualize my gro file. It
looks fine. The polymer chain is a little far away from the nanotube.
There is no overlap. However, after I do mdrun, I can't get edr fil
On Mon, 19 Jun 2006, Guillem Plasencia wrote:
> Then i was curious and did trjconv my system (before running mdrun energy
> minimization) into a pdb, and had a look at it, and i saw my protein was
> splitted in three different molecules, one was inside the water box (but far
> away from box cent
Hi GMX users,
My question is to calculate solvation free energy of a non-standard residue (I
managed to define it into oplsaa database). I followed the tutorial prepared by
groningen group (http://md.chem.rug.nl/education/Free-Energy_Course/index.html)
My problem is how to use dummy atoms in ffop
Hello, I got an error message while using 8 processors becuase of Shake
block crossing node boundaries. Everything was fine when I used a single
processor. Any idea how to ease this problem? Thanks! JW
The error message:
splitting topology...
Walking down the molecule graph to make s
hi,
On Monday 19 June 2006 18:06, Guillem Plasencia wrote:
> Hello,
>
> This is my first MD (besides the ones in GROMACS' benchmark), i found the
> following problem while following John Kerrigan's tutorial for Drug-Enzyme
> complex (the first part, energy minimization), using my own protein and
Dear all,
I had a couple quick questions on the pull code, as I couldn't quite
figure this out from the documentation. In particular, I'm interested
in the part that does umbrella sampling:
1) If an alternative reference structure is provided to grompp using
the -r option (as one would do for po
I have installed GROMACS compiled with MPI support into the /usr/local
directory of ParallelKnoppix. ParallelKnoppix is a Knoppix-like CD that can be
used to set up a Linux cluster in about 5 minutes. I have very little
experience with GROMACS, but I have run some of the demos, and it looks like
Hello,
This is my first MD (besides the ones in GROMACS' benchmark), i found the
following problem while following John Kerrigan's tutorial for Drug-Enzyme
complex (the first part, energy minimization), using my own protein and its
crystallographic ligand i ran into the following:
-briefing
David M.,
Thanks for the suggestions. About the Yu et al. error bars:
> For Yu et
> al., the first number is the average from the full 5 ns simulation and
> the number in () is for the last 2 ns.
If not for the CE23Me case, I would probably assume that the discrepancy due to
doing a notorio
Jonathan,
First, a question: I know that certain values of sc-alpha are preferred for
different cases, but are there any values that definitely should not be used?
In my calculations, some hydrogens (with charges but no L-J) are mutated into
united atom methyls (with charges and L-J), so the
Hello, on this note, I'm having issues configuring and installing the
mpi enabled mdrun. (see below). I keep getting a strange error:
checking size of int... configure: error: cannot compute sizeof
(int), 77
I've pasted the output below, and I've attached the config.log for
reference. I'm rea
Dear, all
I find there are some small molecule's itp file in
/gromacs/share/gromacs/top/; some of them seem belong to united atom
force field, others of them seem belong to all-atom force field.
Now, the question is, most of them has no note about which force field
it belongs to, how can I know wh
hjbai wrote:
> Hi, all
> What's the difference between different force fields? such as gromos 87,
> gromos 96 and opls/aa, I was confused -- How can I get some information
> about this? I have looked through the manual, and cant get a clear
> picture for this problem.
> Thank you, any kinds of disc
Hi, all
What's the difference between different force fields? such as gromos 87,
gromos 96 and opls/aa, I was confused -- How can I get some information
about this? I have looked through the manual, and cant get a clear
picture for this problem.
Thank you, any kinds of discussion will be helpful.
[EMAIL PROTECTED] wrote:
Thank you very much you the advise, I will install fiors LAM and then
MPICH. By the way you think can be interesting to invest in some low
latenci network devices for this little clustter??. Or with the gigabit
Can be enought
Thanks Hector
Of course the scaling wi
Thank you very much you the advise, I will install fiors LAM and then
MPICH. By the way you think can be interesting to invest in some low
latenci network devices for this little clustter??. Or with the gigabit
Can be enought
Thanks Hector
-Original Message-
From: Carsten Kutzner <[
Hello Hector,
since it does not take long to install lam and mpich, I would install
both MPI implementations and then benchmark with a typical MD system
which one performs better.
I would suggest LAM 7.1.2 which is the newest version, and MPICH-2
1.0.3, which works well, at least on our clus
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