Difference between revisions of "Disopred"
(6 intermediate revisions by 2 users not shown) | |||
Line 1: | Line 1: | ||
+ | =DISOPRED= |
||
+ | |||
+ | ==Basic Information== |
||
+ | |||
+ | {| style="float: right; border: 1px solid #BBB; margin: .46em 0 0 .2em;" |
||
+ | ! Author |
||
+ | | Ward JJ, Sodhi JS, McGuffin LJ, Buxton BF, Jones DT |
||
+ | |- |
||
+ | ! Year |
||
+ | | 2004 |
||
+ | |- |
||
+ | ! Reference |
||
+ | | [http://www.ncbi.nlm.nih.gov/pubmed/15019783 PubMed 15019783] |
||
+ | |- |
||
+ | ! ML Method |
||
+ | | SVM |
||
+ | |} |
||
+ | |||
+ | DISOPRED generates a PSI-BLAST profile of the input sequence. A SVM is feeded with a window of 15 residues for each residue of the profile. |
||
+ | This SVM predicts if the residue in the center of the window is in an ordered or disordered region of the protein. |
||
+ | |||
+ | The SVM was trained on 750 non-redundant X-ray structures with high resolution. It was assumed that residues which appear in the sequence but whose coordinates |
||
+ | from the electron density map are missing are in a disordered region of the protein. For each structure was a PSI-Blast profile calculated. These profiles were |
||
+ | used in windows of 15 residues to train a SVM. |
||
+ | This way of defining disordered regions in a protein has its disadvantages, but there are no high-throuput methods to measure disordered regions. |
||
+ | |||
+ | ==FAQ== |
||
+ | ===How to run it locally?=== |
||
Change in the disopred script the following lines: |
Change in the disopred script the following lines: |
||
<nowiki>#</nowiki> Change database location |
<nowiki>#</nowiki> Change database location |
||
+ | |||
set dbane = /data/blast/nr/nr |
set dbane = /data/blast/nr/nr |
||
+ | |||
+ | |||
<nowiki>#</nowiki> Check if there is any path with /usr/local/bin |
<nowiki>#</nowiki> Check if there is any path with /usr/local/bin |
||
+ | |||
change all path to /usr/bin (important: change also the path to the perl location) |
change all path to /usr/bin (important: change also the path to the perl location) |
Latest revision as of 19:41, 5 June 2011
DISOPRED
Basic Information
Author | Ward JJ, Sodhi JS, McGuffin LJ, Buxton BF, Jones DT |
---|---|
Year | 2004 |
Reference | PubMed 15019783 |
ML Method | SVM |
DISOPRED generates a PSI-BLAST profile of the input sequence. A SVM is feeded with a window of 15 residues for each residue of the profile. This SVM predicts if the residue in the center of the window is in an ordered or disordered region of the protein.
The SVM was trained on 750 non-redundant X-ray structures with high resolution. It was assumed that residues which appear in the sequence but whose coordinates from the electron density map are missing are in a disordered region of the protein. For each structure was a PSI-Blast profile calculated. These profiles were used in windows of 15 residues to train a SVM. This way of defining disordered regions in a protein has its disadvantages, but there are no high-throuput methods to measure disordered regions.
FAQ
How to run it locally?
Change in the disopred script the following lines:
# Change database location
set dbane = /data/blast/nr/nr
# Check if there is any path with /usr/local/bin
change all path to /usr/bin (important: change also the path to the perl location)