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hmmsearch(1) HMMER Manual hmmsearch(1)
NAME
hmmsearch - search profile(s) against a sequence database
SYNOPSIS
hmmsearch [options] <hmmfile> <seqdb>
DESCRIPTION
hmmsearch is used to search one or more profiles against a sequence
database. For each profile in <hmmfile>, use that query profile to
search the target database of profiles in <seqdb>, and output ranked
lists of the sequences with the most significant matches to the
profile.
The <hmmfile> may contain more than one profile. To build profiles from
multiple alignments, see hmmbuild.
The output format is designed to be human-readable, but is often so
voluminous that reading it is impractical, and parsing it is a pain.
The --tblout and --domtblout options save output in simple tabular
formats that are concise and easier to parse. The -o option allows
redirecting the main output, including throwing it away in /dev/null.
OPTIONS
-h Help; print a brief reminder of command line usage and all
available options.
OPTIONS FOR CONTROLLING OUTPUT
-o <f> Direct the main human-readable output to a file <f> instead of
the default stdout.
-A <f> Save a multiple alignment of all significant hits (those
satisfying inclusion thresholds) to the file <f>.
--tblout <f>
Save a simple tabular (space-delimited) file summarizing the
per-target output, with one data line per homologous target
sequence found.
--domtblout <f>
Save a simple tabular (space-delimited) file summarizing the
per-domain output, with one data line per homologous domain
detected in a query sequence for each homologous model.
--acc Use accessions instead of names in the main output, where
available for profiles and/or sequences.
--noali
Omit the alignment section from the main output. This can
greatly reduce the output volume.
--notextw
Unlimit the length of each line in the main output. The default
is a limit of 120 characters per line, which helps in displaying
the output cleanly on terminals and in editors, but can truncate
target profile description lines.
--textw <n>
Set the main output's line length limit to <n> characters per
line. The default is 120.
OPTIONS CONTROLLING REPORTING THRESHOLDS
Reporting thresholds control which hits are reported in output files
(the main output, --tblout, and --domtblout). Sequence hits and domain
hits are ranked by statistical significance (E-value) and output is
generated in two sections called per-target and per-domain output. In
per-target output, by default, all sequence hits with an E-value <= 10
are reported. In the per-domain output, for each target that has passed
per-target reporting thresholds, all domains satisfying per-domain
reporting thresholds are reported. By default, these are domains with
conditional E-values of <= 10. The following options allow you to
change the default E-value reporting thresholds, or to use bit score
thresholds instead.
-E <x> In the per-target output, report target sequences with an E-
value of <= <x>. The default is 10.0, meaning that on average,
about 10 false positives will be reported per query, so you can
see the top of the noise and decide for yourself if it's really
noise.
-T <x> Instead of thresholding per-profile output on E-value, instead
report target sequences with a bit score of >= <x>.
--domE <x>
In the per-domain output, for target sequences that have already
satisfied the per-profile reporting threshold, report individual
domains with a conditional E-value of <= <x>. The default is
10.0. A conditional E-value means the expected number of
additional false positive domains in the smaller search space of
those comparisons that already satisfied the per-target
reporting threshold (and thus must have at least one homologous
domain already).
--domT <x>
Instead of thresholding per-domain output on E-value, instead
report domains with a bit score of >= <x>.
OPTIONS FOR INCLUSION THRESHOLDS
Inclusion thresholds are stricter than reporting thresholds. Inclusion
thresholds control which hits are considered to be reliable enough to
be included in an output alignment or a subsequent search round, or
marked as significant ("!") as opposed to questionable ("?") in domain
output.
--incE <x>
Use an E-value of <= <x> as the per-target inclusion threshold.
The default is 0.01, meaning that on average, about 1 false
positive would be expected in every 100 searches with different
query sequences.
--incT <x>
Instead of using E-values for setting the inclusion threshold,
instead use a bit score of >= <x> as the per-target inclusion
threshold. By default this option is unset.
--incdomE <x>
Use a conditional E-value of <= <x> as the per-domain inclusion
threshold, in targets that have already satisfied the overall
per-target inclusion threshold. The default is 0.01.
--incdomT <x>
Instead of using E-values, use a bit score of >= <x> as the per-
domain inclusion threshold.
OPTIONS FOR MODEL-SPECIFIC SCORE THRESHOLDING
Curated profile databases may define specific bit score thresholds for
each profile, superseding any thresholding based on statistical
significance alone.
To use these options, the profile must contain the appropriate (GA, TC,
and/or NC) optional score threshold annotation; this is picked up by
hmmbuild from Stockholm format alignment files. Each thresholding
option has two scores: the per-sequence threshold <x1> and the per-
domain threshold <x2> These act as if -T<x1> --incT<x1> --domT<x2>
--incdomT<x2> has been applied specifically using each model's curated
thresholds.
--cut_ga
Use the GA (gathering) bit scores in the model to set per-
sequence (GA1) and per-domain (GA2) reporting and inclusion
thresholds. GA thresholds are generally considered to be the
reliable curated thresholds defining family membership; for
example, in Pfam, these thresholds define what gets included in
Pfam Full alignments based on searches with Pfam Seed models.
--cut_nc
Use the NC (noise cutoff) bit score thresholds in the model to
set per-sequence (NC1) and per-domain (NC2) reporting and
inclusion thresholds. NC thresholds are generally considered to
be the score of the highest-scoring known false positive.
--cut_tc
Use the NC (trusted cutoff) bit score thresholds in the model to
set per-sequence (TC1) and per-domain (TC2) reporting and
inclusion thresholds. TC thresholds are generally considered to
be the score of the lowest-scoring known true positive that is
above all known false positives.
OPTIONS CONTROLLING THE ACCELERATION PIPELINE
HMMER3 searches are accelerated in a three-step filter pipeline: the
MSV filter, the Viterbi filter, and the Forward filter. The first
filter is the fastest and most approximate; the last is the full
Forward scoring algorithm. There is also a bias filter step between MSV
and Viterbi. Targets that pass all the steps in the acceleration
pipeline are then subjected to postprocessing -- domain identification
and scoring using the Forward/Backward algorithm.
Changing filter thresholds only removes or includes targets from
consideration; changing filter thresholds does not alter bit scores, E-
values, or alignments, all of which are determined solely in
postprocessing.
--max Turn off all filters, including the bias filter, and run full
Forward/Backward postprocessing on every target. This increases
sensitivity somewhat, at a large cost in speed.
--F1 <x>
Set the P-value threshold for the MSV filter step. The default
is 0.02, meaning that roughly 2% of the highest scoring
nonhomologous targets are expected to pass the filter.
--F2 <x>
Set the P-value threshold for the Viterbi filter step. The
default is 0.001.
--F3 <x>
Set the P-value threshold for the Forward filter step. The
default is 1e-5.
--nobias
Turn off the bias filter. This increases sensitivity somewhat,
but can come at a high cost in speed, especially if the query
has biased residue composition (such as a repetitive sequence
region, or if it is a membrane protein with large regions of
hydrophobicity). Without the bias filter, too many sequences may
pass the filter with biased queries, leading to slower than
expected performance as the computationally intensive
Forward/Backward algorithms shoulder an abnormally heavy load.
OTHER OPTIONS
--nonull2
Turn off the null2 score corrections for biased composition.
-Z <x> Assert that the total number of targets in your searches is <x>,
for the purposes of per-sequence E-value calculations, rather
than the actual number of targets seen.
--domZ <x>
Assert that the total number of targets in your searches is <x>,
for the purposes of per-domain conditional E-value calculations,
rather than the number of targets that passed the reporting
thresholds.
--seed <n>
Set the random number seed to <n>. Some steps in postprocessing
require Monte Carlo simulation. The default is to use a fixed
seed (42), so that results are exactly reproducible. Any other
positive integer will give different (but also reproducible)
results. A choice of 0 uses a randomly chosen seed.
--qformat <s>
Assert that the query sequence file is in format <s>. Accepted
formats include fasta, embl, genbank, ddbj, uniprot, stockholm,
pfam, a2m, and afa. The default is to autodetect the format of
the file.
--cpu <n>
Set the number of parallel worker threads to <n>. By default,
HMMER sets this to the number of CPU cores it detects in your
machine - that is, it tries to maximize the use of your
available processor cores. Setting <n> higher than the number of
available cores is of little if any value, but you may want to
set it to something less. You can also control this number by
setting an environment variable, HMMER_NCPU.
This option is only available if HMMER was compiled with POSIX
threads support. This is the default, but it may have been
turned off at compile-time for your site or machine for some
reason.
--stall
For debugging the MPI master/worker version: pause after start,
to enable the developer to attach debuggers to the running
master and worker(s) processes. Send SIGCONT signal to release
the pause. (Under gdb: (gdb) signal SIGCONT) (Only available if
optional MPI support was enabled at compile-time.)
--mpi Run in MPI master/worker mode, using mpirun. (Only available if
optional MPI support was enabled at compile-time.)
SEE ALSO
See hmmer(1) for a master man page with a list of all the individual
man pages for programs in the HMMER package.
For complete documentation, see the user guide that came with your
HMMER distribution (Userguide.pdf); or see the HMMER web page
(@HMMER_URL@).
COPYRIGHT
@HMMER_COPYRIGHT@
@HMMER_LICENSE@
For additional information on copyright and licensing, see the file
called COPYRIGHT in your HMMER source distribution, or see the HMMER
web page (@HMMER_URL@).
AUTHOR
Eddy/Rivas Laboratory
Janelia Farm Research Campus
19700 Helix Drive
Ashburn VA 20147 USA
http://eddylab.org
HMMER @HMMER_VERSION@ @HMMER_DATE@ hmmsearch(1)