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This is the command progressiveMauve that can be run in the OnWorks free hosting provider using one of our multiple free online workstations such as Ubuntu Online, Fedora Online, Windows online emulator or MAC OS online emulator

PROGRAM:

NAME


progressiveMauve - efficiently constructing multiple genome alignments

DESCRIPTION


progressiveMauve usage:

When each genome resides in a separate file: progressiveMauve [options] <seq1 filename>
... <seqN filename>

When all genomes are in a single file: progressiveMauve [options] <seq filename>

OPTIONS


--island-gap-size=<number> Alignment gaps above this size in nucleotides are considered to
be islands [20]

--profile=<file> (Not yet implemented) Read an existing sequence alignment in XMFA format
and align it to other sequences or alignments

--apply-backbone=<file> Read an existing sequence alignment in XMFA format and apply
backbone statistics to it

--disable-backbone Disable backbone detection

--mums Find MUMs only, do not attempt to determine locally collinear blocks (LCBs)

--seed-weight=<number> Use the specified seed weight for calculating initial anchors

--output=<file> Output file name.
Prints to screen by default

--backbone-output=<file> Backbone output file name (optional).

--match-input=<file> Use specified match file instead of searching for matches

--input-id-matrix=<file> An identity matrix describing similarity among all pairs of input
sequences/alignments

--max-gapped-aligner-length=<number> Maximum number of base pairs to attempt aligning with
the gapped aligner

--input-guide-tree=<file> A phylogenetic guide tree in NEWICK format that describes the
order in which sequences will be aligned

--output-guide-tree=<file> Write out the guide tree used for alignment to a file

--version Display software version information

--debug Run in debug mode (perform internal consistency checks--very slow)

--scratch-path-1=<path> Designate a path that can be used for temporary data storage.
Two or more paths should be specified.

--scratch-path-2=<path> Designate a path that can be used for temporary data storage.
Two or more paths should be specified.

--collinear Assume that input sequences are collinear--they have no rearrangements

--scoring-scheme=<ancestral|sp_ancestral|sp> Selects the anchoring score function.
Default is extant sum-of-pairs (sp).

--no-weight-scaling Don't scale LCB weights by conservation distance and breakpoint
distance

--max-breakpoint-distance-scale=<number [0,1]> Set the maximum weight scaling by
breakpoint distance.
Defaults to 0.5

--conservation-distance-scale=<number [0,1]> Scale conservation distances by this amount.
Defaults to 0.5

--muscle-args=<arguments in quotes> Additional command-line options for MUSCLE.
Any quotes should be escaped with a backslash

--skip-refinement Do not perform iterative refinement

--skip-gapped-alignment Do not perform gapped alignment

--bp-dist-estimate-min-score=<number> Minimum LCB score for estimating pairwise breakpoint
distance

--mem-clean Set this to true when debugging memory allocations

--gap-open=<number> Gap open penalty

--repeat-penalty=<negative|zero> Sets whether the repeat scores go negative or go to zero
for highly repetitive sequences.
Default is negative.

--gap-extend=<number> Gap extend penalty

--substitution-matrix=<file> Nucleotide substitution matrix in NCBI format

--weight=<number> Minimum pairwise LCB score

--min-scaled-penalty=<number> Minimum breakpoint penalty after scaling the penalty by
expected divergence

--hmm-p-go-homologous=<number> Probability of transitioning from the unrelated to the
homologous state [0.00001]

--hmm-p-go-unrelated=<number> Probability of transitioning from the homologous to the
unrelated state [0.000000001]

--hmm-identity=<number> Expected level of sequence identity among pairs of sequences,
ranging between 0 and 1 [0.7]

--seed-family Use a family of spaced seeds to improve sensitivity

--solid-seeds Use solid seeds. Do not permit substitutions in anchor matches.

--coding-seeds Use coding pattern seeds. Useful to generate matches coding regions with
3rd codon position degeneracy.

--disable-cache Disable recursive anchor search cacheing to workaround a crash bug

--no-recursion Disable recursive anchor search

EXAMPLES


progressiveMauve --output=my_seqs.xmfa my_genome1.gbk my_genome2.gbk my_genome3.fasta

If genomes are in a single file and have no rearrangement: progressiveMauve --collinear
--output=my_seqs.xmfa my_genomes.fasta

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