ZINC:FAQ: Difference between revisions
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sed -e 's/^/fget2.pl?f=m\&l=0\&z=/' codes > codes2 | sed -e 's/^/fget2.pl?f=m\&l=0\&z=/' codes > codes2 | ||
wget -O all.mol2 -a listing -B http://zinc8.docking.org/ -i codes2 | wget -O all.mol2 -a listing -B http://zinc8.docking.org/ -i codes2 | ||
Note this currently only gets a single (pH 7) representation of each molecule. | |||
[[Category:FAQ]] | [[Category:FAQ]] | ||
[[Category:ZINC]] | [[Category:ZINC]] |
Revision as of 22:27, 6 December 2007
Here are frequently asked questions about ZINC.
Q1. I am trying to generate a subset of your "drug-like" molecule subset for
virtual screening. I was thinking your 60% diversity group (about 12,000
molecules) would be a place to start, and I downloaded the .smi file. I
relatively new to chemoinformatics and I was wondering if there is an
elegant way to separate the compounds listed in the .smi file from the
larger library containing the mol2 files from the 2,000,000 "usual" set that
I have downloaded from ZINC?
A1.
wget http://zinc8.docking.org/subset1/3/3_t60.smi awk '{print $2}' 3_t60.smi >! codes sed -e 's/^/fget2.pl?f=m\&l=0\&z=/' codes > codes2 wget -O all.mol2 -a listing -B http://zinc8.docking.org/ -i codes2
Note this currently only gets a single (pH 7) representation of each molecule.