[modeller_usage] Frustrating simple problem!

[Joel Tyndall <>]

Hi folks,

I've got a frustrating problem when I try to run a modeller job. I know 
it  works as I've used it previously. I have seen the error before on 
the bulletin board but can't find the cause of my problem.

I get the error:

read_al_375E> Unknown residue type,position,sequence:          1        1

I don't have any alt conformations. any help would be great. I have 
attached the top and ali files.

Cheers

J

--
Joel Tyndall, PhD

Lecturer
National School of Pharmacy
University of Otago 
PO Box 913 Dunedin 
New Zealand 
Ph +64 3 4797293 
Fax +64 3 4797034

>P1;UP_ecoli
structureX:1rxc:1     : :253  : :unknown:unknown:-1.00:-1.00
MSKSDVFHLGLTKN------DLQGATLAIVPGDPDRVEKIAALMDKPVKLAS-HREFTTW
RAELD------GKPVIVCSTGIGGPSTSIAVEELAQLG------IRTFLRIGTTGAIQPH
INVGDVLVTTASVR------LDGASLHFAPLEFPAVADFECTTALVEAAKSIGATTHVGV
TASSDTFYPGQERYD-TYSGRVVRHFKGSMEEWQAMGVMNYEMESATLLTMCASQGLRAG
MVAGVIVNRTQQEIPN--AETMKQTESHAVKIVVEAARRLL*
>P1;1uph
sequence:uph:1   : :282  : :unknown:unknown:-1.00:-1.00
MKEDILYHFNLTTSRHNFPALFGDVKFVCVGGSPSRMKAFIRCVGAELGLDCPGRDYPNI
CAGTDRYAMYKVGPVLSVSHGMGIPSISIMLHELIKLLYYARCSNVTIIRIGTSGGIG--
LEPGTVVITEQAVDTCFKAEFEQIVLGKRVIRKTDLNKKLVQELLLCSAELSEFTTVVGN
TMCTLDFYEGQGRLDGALCSYTEKDKQAYLEAAYAAGVRNIEMESSVFAAMCSACGLQAA
VVCVTLLNRLEGDQISSPRNVLSEYQQRPQRLVSYFIKKKL*

                         MODELLER 6v2, 17 Feb 2002

     PROTEIN STRUCTURE MODELLING BY SATISFACTION OF SPATIAL RESTRAINTS

                                                                 
                     Copyright(c) 1989-2002 Andrej Sali          
                            All Rights Reserved                  
                                                                 
                            Written by A. Sali                   
          with help from A. Fiser, R. Sanchez, M.A. Marti-Renom, 
                   B. Jerkovic, A. Badretdinov, F. Melo,         
                       J.P. Overington & E. Feyfant              
                   Rockefeller University, New York, USA         
                     Harvard University, Cambridge, USA          
                 Imperial Cancer Research Fund, London, UK       
             Birkbeck College, University of London, London, UK  


Kind, OS, HostName, Kernel, Processor: 4, Linux allroy.otago.ac.nz 2.6.5-1.358smp x86_64
Date and time of compilation         : 07/16/2002 11:42:16
Job starting time (YY/MM/DD HH:MM:SS): 2004/10/29  16:08:43.499

TOP_________>   106  706 SET ALNFILE               = 'UP_human_ecoli' 
 
TOP_________>   107  707 SET KNOWNS                = '1rxc_mono' 
 
TOP_________>   108  708 SET MD_LEVEL              = 'refine_3' 
 
TOP_________>   109  709 SET SEQUENCE              = '1uph' 
 
TOP_________>   110  710 SET ATOM_FILES_DIRECTORY  = './:../atom_files' 
 
TOP_________>   111  711 SET OUTPUT_DIRECTORY      = './' 
 
TOP_________>   112  712 SET PDB_EXT               = '.pdb' 
 
TOP_________>   113  713 SET ALIGNMENT_FORMAT    = 'PIR' 
 
TOP_________>   114  714 SET STARTING_MODEL        = 1 
 
TOP_________>   115  715 SET ENDING_MODEL          = 5 
 
TOP_________>   116  716 SET DEVIATION             = 4.000000 
 
TOP_________>   117  717 SET FINAL_MALIGN3D        = 1 
 
TOP_________>   118  718 SET DO_LOOPS = 1 
 
TOP_________>   119  719 SET RADII_FACTOR          = 0.915 
 
TOP_________>   120  720 SET LOOP_STARTING_MODEL = 1 
 
TOP_________>   121  721 SET LOOP_ENDING_MODEL   = 5 
 
TOP_________>   122  722 SET LOOP_MD_LEVEL = 'refine_2' 
 
TOP_________>   123  723 CALL ROUTINE            = 'model' 
 
TOP_________>   124  399 CALL ROUTINE = 'getnames' 
 
TOP_________>   125  509 STRING_IF STRING_ARGUMENTS = MODEL 'undefined', OPERATION;
                       = 'EQ', THEN =     'STRING_OPERATE OPERATION = CONCATENA;
                      TE, STRING_ARGUMENTS = SEQUENCE .ini, RESULT = MODEL' 
 
TOP_________>   126  510 STRING_IF STRING_ARGUMENTS = CSRFILE 'undefined', OPERATI;
                      ON = 'EQ', THEN =     'STRING_OPERATE OPERATION = CONCATE;
                      NATE, STRING_ARGUMENTS = SEQUENCE .rsr,  RESULT = CSRFILE;
                      ' 
 
TOP_________>   127  511 STRING_OPERATE OPERATION = 'CONCATENATE',                ;
                         STRING_ARGUMENTS = SEQUENCE '.sch',  RESULT = SCHFILE 
 
TOP_________>   128  512 STRING_OPERATE OPERATION = 'CONCATENATE',                ;
                        STRING_ARGUMENTS = SEQUENCE '.mat',  RESULT = MATRIX_FI;
                      LE 
 
TOP_________>   129  513 SET ROOT_NAME = SEQUENCE 
 
TOP_________>   130  514 RETURN 
 
TOP_________>   131  400 CALL ROUTINE = 'homcsr' 
 
TOP_________>   132  106 READ_ALIGNMENT FILE = ALNFILE, ALIGN_CODES = KNOWNS SEQUE;
                      NCE 
 

Dynamically allocated memory at         amaxseq [B,kB,MB]:      2205269    2153.583     2.103
openf5__224_> Open       11  OLD  SEQUENTIAL  UP_human_ecoli.ali

Dynamically allocated memory at         amaxbnd [B,kB,MB]:      6262261    6115.489     5.972
openf5__224_> Open       11  OLD  SEQUENTIAL  UP_human_ecoli.ali
read_al_375E> Unknown residue type,position,sequence:          1        1
recover____E> ERROR_STATUS >= STOP_ON_ERROR:        1       1

Dynamically allocated memory at          finish [B,kB,MB]:      6262261    6115.489     5.972
Starting time                                            : 2004/10/29  16:08:43.499
Closing time                                             : 2004/10/29  16:08:44.900
Total CPU time [seconds]                                 :       1.38

INCLUDE        # remove all the #'d bits. TOP FILE FOR EXTENSIVE REFINEMENT

SET INITIAL_MALIGN3D = 1                   # don't worry about this.
SET OUTPUT_CONTROL = 1 1 1 1 1             # don't worry about this either
SET ALNFILE               = 'UP_human_ecoli' # alignment file, worry about this
SET KNOWNS                = '1rxc_mono'    # refers to xtal name in algnmnt
SET MD_LEVEL              = 'refine_3'     # sets simulated annealing level 1 high 3 low. 3 good to tansfer coords and fix major gliches.
SET SEQUENCE              = '1uph'         # name of target seq in pir file
SET ATOM_FILES_DIRECTORY  = './:../atom_files' # for modeller use. It will tell you if it can't find its atoms.
SET OUTPUT_DIRECTORY      = './'           # is exactly that; can alter this
SET PDB_EXT               = '.pdb'         # leave all structures as this
SET ALIGNMENT_FORMAT 	= 'PIR'            # leave it this way; easier
SET STARTING_MODEL        = 1              # these two define the number of
SET ENDING_MODEL          = 5              # models to build. Unclear why it is this way
SET DEVIATION             = 4.000000       # defines how much variation is tolerated when building your model from the randomised coords. Leave as is.
SET FINAL_MALIGN3D        = 1              # don't worry about this
SET DO_LOOPS = 1                           # for explicit loop building
SET RADII_FACTOR          = 0.915          # the x factor for good structure. Always include this.
 SET LOOP_STARTING_MODEL = 1               #back to explicit loop modeling
 SET LOOP_ENDING_MODEL   = 5               # i built 10 per model, 50 loops in total. Too much. 1 model 10 loops
 SET LOOP_MD_LEVEL = 'refine_2'            # md level used; same as above
CALL ROUTINE            = 'model'          # is the modeller key word for modelling building