patmatmotifs.txt

emboss的linux版本的源代码

                               patmatmotifs 



Function

   Search a PROSITE motif database with a protein sequence

Description

   patmatmotifs takes a protein sequence and compares it to the PROSITE
   database of motifs.

   For a description of PROSITE, we can do no better than to quote the
   PROSITE user's documentation: 

   PROSITE is a method of determining what is the function of
   uncharacterized proteins translated from genomic or cDNA sequences. It
   consists of a database of biologically significant sites and patterns
   formulated in such a way that with appropriate computational tools it
   can rapidly and reliably identify to which known family of protein (if
   any) the new sequence belongs.

   In some cases the sequence of an unknown protein is too distantly
   related to any protein of known structure to detect its resemblance by
   overall sequence alignment, but it can be identified by the occurrence
   in its sequence of a particular cluster of residue types which is
   variously known as a pattern, motif, signature, or fingerprint. These
   motifs arise because of particular requirements on the structure of
   specific region(s) of a protein which may be important, for example,
   for their binding properties or for their enzymatic activity. These
   requirements impose very tight constraints on the evolution of those
   limited (in size) but important portion(s) of a protein sequence. To
   paraphrase Orwell, in Animal Farm, we can say that "some regions of a
   protein sequence are more equal than others" !

   The use of protein sequence patterns (or motifs) to determine the
   function(s) of proteins is becoming very rapidly one of the essential
   tools of sequence analysis. This reality has been recognized by many
   authors, as it can be illustrated from the following citations from
   two of the most well known experts of protein sequence analysis, R.F.
   Doolittle and A.M. Lesk:
      "There are  many short  sequences  that  are  often  (but  not  always)
      diagnostics of certain binding properties or active sites. These can be
      set into a small subcollection and searched against your sequence (1)".

      "In some  cases, the structure and function of an unknown protein which
      is too  distantly related  to any  protein of known structure to detect
      its affinity  by overall  sequence alignment  may be  identified by its
      possession of  a particular  cluster of  residues types classified as a
      motifs. The  motifs, or  templates, or  fingerprints, arise  because of
      particular  requirements  of  binding  sites  that  impose  very  tight
      constraint on the evolution of portions of a protein sequence (2)."

   The home web page of PROSITE is: http://www.expasy.ch/prosite/

   It is common to find that a search of the PROSITE database against a
   protein sequence will report many matches to the short motifs that are
   indicative of the post-translational modification sites, such as
   glycolsylation, myristylation and phosphorylation sites. These reports
   are often unwanted and are not normally reported. You can turn
   reporting of these short motifs on by giving the '-noprune' option on
   the command-line.

   Your EMBOSS administrator must have set up the local EMBOSS PROSITE
   database using the utility 'prosextract' before this program will run.

Usage

   Here is a sample session with patmatmotifs


% patmatmotifs -full 
Search a PROSITE motif database with a protein sequence
Input protein sequence: tsw:opsd_human
Output report [opsd_human.patmatmotifs]: 

   Go to the input files for this example
   Go to the output files for this example

Command line arguments

   Standard (Mandatory) qualifiers:
  [-sequence]          sequence   Protein sequence filename and optional
                                  format, or reference (input USA)
  [-outfile]           report     [*.patmatmotifs] Output report file name

   Additional (Optional) qualifiers:
   -full               boolean    [N] Provide full documentation for matching
                                  patterns
   -[no]prune          boolean    [Y] Ignore simple patterns. If this is true
                                  then these simple post-translational
                                  modification sites are not reported:
                                  myristyl, asn_glycosylation,
                                  camp_phospho_site, pkc_phospho_site,
                                  ck2_phospho_site, and tyr_phospho_site.

   Advanced (Unprompted) qualifiers: (none)
   Associated qualifiers:

   "-sequence" associated qualifiers
   -sbegin1            integer    Start of the sequence to be used
   -send1              integer    End of the sequence to be used
   -sreverse1          boolean    Reverse (if DNA)
   -sask1              boolean    Ask for begin/end/reverse
   -snucleotide1       boolean    Sequence is nucleotide
   -sprotein1          boolean    Sequence is protein
   -slower1            boolean    Make lower case
   -supper1            boolean    Make upper case
   -sformat1           string     Input sequence format
   -sdbname1           string     Database name
   -sid1               string     Entryname
   -ufo1               string     UFO features
   -fformat1           string     Features format
   -fopenfile1         string     Features file name

   "-outfile" associated qualifiers
   -rformat2           string     Report format
   -rname2             string     Base file name
   -rextension2        string     File name extension
   -rdirectory2        string     Output directory
   -raccshow2          boolean    Show accession number in the report
   -rdesshow2          boolean    Show description in the report
   -rscoreshow2        boolean    Show the score in the report
   -rusashow2          boolean    Show the full USA in the report
   -rmaxall2           integer    Maximum total hits to report
   -rmaxseq2           integer    Maximum hits to report for one sequence

   General qualifiers:
   -auto               boolean    Turn off prompts
   -stdout             boolean    Write standard output
   -filter             boolean    Read standard input, write standard output
   -options            boolean    Prompt for standard and additional values
   -debug              boolean    Write debug output to program.dbg
   -verbose            boolean    Report some/full command line options
   -help               boolean    Report command line options. More
                                  information on associated and general
                                  qualifiers can be found with -help -verbose
   -warning            boolean    Report warnings
   -error              boolean    Report errors
   -fatal              boolean    Report fatal errors
   -die                boolean    Report dying program messages

Input file format

   patmatmotifs reads a protein sequence USA.

  Input files for usage example

   'tsw:opsd_human' is a sequence entry in the example protein database
   'tsw'

  Database entry: tsw:opsd_human

ID   OPSD_HUMAN     STANDARD;      PRT;   348 AA.
AC   P08100; Q16414;
DT   01-AUG-1988 (Rel. 08, Created)
DT   01-AUG-1988 (Rel. 08, Last sequence update)
DT   15-JUL-1999 (Rel. 38, Last annotation update)
DE   RHODOPSIN.
GN   RHO.
OS   Homo sapiens (Human).
OC   Eukaryota; Metazoa; Chordata; Craniata; Vertebrata; Mammalia;
OC   Eutheria; Primates; Catarrhini; Hominidae; Homo.
RN   [1]
RP   SEQUENCE FROM N.A.
RX   MEDLINE; 84272729.
RA   NATHANS J., HOGNESS D.S.;
RT   "Isolation and nucleotide sequence of the gene encoding human
RT   rhodopsin.";
RL   Proc. Natl. Acad. Sci. U.S.A. 81:4851-4855(1984).
RN   [2]
RP   SEQUENCE OF 1-120 FROM N.A.
RA   BENNETT J., BELLER B., SUN D., KARIKO K.;
RL   Submitted (NOV-1994) to the EMBL/GenBank/DDBJ databases.
RN   [3]
RP   REVIEW ON ADRP VARIANTS.
RX   MEDLINE; 94004905.
RA   AL-MAGHTHEH M., GREGORY C., INGLEHEARN C., HARDCASTLE A.,
RA   BHATTACHARYA S.;
RT   "Rhodopsin mutations in autosomal dominant retinitis pigmentosa.";
RL   Hum. Mutat. 2:249-255(1993).
RN   [4]
RP   VARIANT ADRP HIS-23.
RX   MEDLINE; 90136922.
RA   DRYJA T.P., MCGEE T.L., REICHEI E., HAHN L.B., COWLEY G.S.,
RA   YANDELL D.W., SANDBERG M.A., BERSON E.L.;
RT   "A point mutation of the rhodopsin gene in one form of retinitis
RT   pigmentosa.";
RL   Nature 343:364-366(1990).
RN   [5]
RP   VARIANTS ADRP.
RX   MEDLINE; 91051574.
RA   FARRAR G.J., KENNA P., REDMOND R., MCWILLIAM P., BRADLEY D.G.,
RA   HUMPHRIES M.M., SHARP E.M., INGLEHEARN C.F., BASHIR R., JAY M.,
RA   WATTY A., LUDWIG M., SCHINZEL A., SAMANNS C., GAL A.,
RA   BHATTACHARYA S.S., HUMPHRIES P.;
RT   "Autosomal dominant retinitis pigmentosa: absence of the rhodopsin
RT   proline-->histidine substitution (codon 23) in pedigrees from
RT   Europe.";
RL   Am. J. Hum. Genet. 47:941-945(1990).
RN   [6]
RP   VARIANTS ADRP HIS-23; ARG-58; LEU-347 AND SER-347.
RX   MEDLINE; 91015273.


  [Part of this file has been deleted for brevity]

FT                                /FTId=VAR_004816.
FT   VARIANT     209    209       V -> M (EFFECT NOT KNOWN).
FT                                /FTId=VAR_004817.
FT   VARIANT     211    211       H -> P (IN ADRP).
FT                                /FTId=VAR_004818.
FT   VARIANT     211    211       H -> R (IN ADRP).
FT                                /FTId=VAR_004819.
FT   VARIANT     216    216       M -> K (IN ADRP).
FT                                /FTId=VAR_004820.
FT   VARIANT     220    220       F -> C (IN ADRP).
FT                                /FTId=VAR_004821.
FT   VARIANT     222    222       C -> R (IN ADRP).
FT                                /FTId=VAR_004822.
FT   VARIANT     255    255       MISSING (IN ADRP).
FT                                /FTId=VAR_004823.
FT   VARIANT     264    264       MISSING (IN ADRP).
FT                                /FTId=VAR_004824.
FT   VARIANT     267    267       P -> L (IN ADRP).
FT                                /FTId=VAR_004825.
FT   VARIANT     267    267       P -> R (IN ADRP).
FT                                /FTId=VAR_004826.
FT   VARIANT     292    292       A -> E (IN CSNB4).
FT                                /FTId=VAR_004827.
FT   VARIANT     296    296       K -> E (IN ADRP).
FT                                /FTId=VAR_004828.
FT   VARIANT     297    297       S -> R (IN ADRP).
FT                                /FTId=VAR_004829.
FT   VARIANT     342    342       T -> M (IN ADRP).
FT                                /FTId=VAR_004830.
FT   VARIANT     345    345       V -> L (IN ADRP).
FT                                /FTId=VAR_004831.
FT   VARIANT     345    345       V -> M (IN ADRP).
FT                                /FTId=VAR_004832.
FT   VARIANT     347    347       P -> A (IN ADRP).
FT                                /FTId=VAR_004833.
FT   VARIANT     347    347       P -> L (IN ADRP; COMMON VARIANT).
FT                                /FTId=VAR_004834.
FT   VARIANT     347    347       P -> Q (IN ADRP).