Re: [AMBER] Problem compatibility pdb in tleap from Daniel Roe on 2013-01-23 (Amber Archive Jan 2013)

From: Daniel Roe <daniel.r.roe.gmail.com>
Date: Wed, 23 Jan 2013 14:41:30 -0700

Hi,

I can think of two ways you might do this. You can try using cpptraj
to write the frame directly, which should write the proper TER cards
and atom/residue names. Alternatively, use ptraj/cpptraj to write out
the specified frame as an amber restart, then use ambpdb to convert
that restart to a PDB file.

-Dan

On Wed, Jan 23, 2013 at 2:32 PM, Stefan Knippenberg
<Stefan.Knippenberg.umons.ac.be> wrote:
> Hi everybody,
>
> >From your answers, I understood I should have loaded a mol2 file - thanks for the suggestion (loadmol2 mol.mol2).
> But still, it does not work and the problem in tleap ("Created a new atom named: C165 within residue: .R<0 1>") is the same...
>
> The pdb I spoke about below was created using ptraj. I do not understand how I can use ambpdb to take frame 942 from the .mdcrd file.
>
> Any further ideas? With (small) molecules, I would try antechamber, but I cannot use it here (DNA+nonstandard molecule)...
>
> Thanks for any help!
>
> Bye,
>
> Stefan
>
>
> ________________________________________
> From: David A Case [case.biomaps.rutgers.edu]
> Sent: 23 January 2013 19:55
> To: AMBER Mailing List
> Subject: Re: [AMBER] Problem compatibility pdb in tleap
>
> On Wed, Jan 23, 2013, Stefan Knippenberg wrote:
>>
>> Willing to solvate a system which has been running in production run for
>> something like 100 ns, I got stuck by reading the pdb file in tleap:
>>
>> Created a new atom named: C165 within residue: .R<0 1>
>
> You don't say how you made the pdb file.
>
>> The pdb I started from is the final structure of a previous calculation,
>> and reads like
>>
>> ATOM 233 7C16 0 1 171.290 58.160 51.330 0.00 0.00
>
> But no standard amino acids or nucleic acids have atoms names like the above,
> and you have a residue named "0" (zero), rather than a real residue name. So,
> you will have to correctly generate a pdb file (use ambpdb), and you will have
> to load the topology library (.lib, .mol2 or similar file) for the
> non-standard residue. It is not enough just to load the frcmod file.
>
> ...dac
>
>
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-- 
-------------------------
Daniel R. Roe, PhD
Department of Medicinal Chemistry
University of Utah
30 South 2000 East, Room 201
Salt Lake City, UT 84112-5820
http://home.chpc.utah.edu/~cheatham/
(801) 587-9652
(801) 585-9119 (Fax)
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Received on Wed Jan 23 2013 - 14:00:03 PST