codcmp Wiki The master copies of EMBOSS documentation are available at http://emboss.open-bio.org/wiki/Appdocs on the EMBOSS Wiki. Please help by correcting and extending the Wiki pages. Function Codon usage table comparison Description codcmp reads two codon usage table files and writes to file the differences in codon usage fractions between the two tables. The usage fraction of a codon is its proportion (0 to 1) of the total number of the codons in the sequences used to construct the usage table. For each codon that is used in both tables, it takes the difference between the usage fractions in the two tables. The sum of the differences and the sum of the differences squared is reported in the output file. It also counts the number of the 64 possible codons which are unused (i.e. has a usage fraction of 0) in either one or the other or both of the codon usage tables, and writes this to the output file. Statistical significance Question: How do you interpret the statistical significance of any difference between the tables? Answer: This is a very interesting question. I don't think that there is any way to say if it is statistically significant just from looking at it, as it is essentially a descriptive statistic about the difference between two 64-mer vectors. If you have a whole lot of sequences and codcmp results for all the possible pairwise comparisons, then the resulting distance matrix can be used to build a phylogenetic tree based on codon usage. However, if you generate a series of random sequences, measure their codon usage and then do codcmp between each of your test sequences and all the random sequences, you could then use a z-test to see if the result between the two test sequences was outside of the top or bottom 5%. This would assume that the codcmp results were normally distributed, but you could test that too. The simplest way is just to plot them and look for a bell-curve. For more rigour, find the mean and standard deviation of your results from the random sequences, use the normal distribution equation to generate a theoretical distribution for that mean and standard deviation, and then perform a chi square between the random data and the theoretically generated normal distribution. If you generate two sets of random data, each based on your two test sequences, an F-test should be used to establish that they have equal variances. Then you can safely go ahead and perform the z-test. You could use shuffle to base your random sequences on the test sequences - so that would ensure the randomised background had the same nucleotide content. F-tests, z-tests and chi-tests can all be done in Excel, as well as being standard in most statistical analysis packages. Answered by Derek Gatherer 21 Nov 2003 Usage Here is a sample session with codcmp This compares the codon usage tables for Escherichia coli and Haemophilus influenzae. % codcmp Codon usage table comparison Codon usage file: Eecoli.cut Second Codon usage file: Ehaein.cut Output file [eecoli.codcmp]: Go to the output files for this example Command line arguments Codon usage table comparison Version: EMBOSS:6.4.0.0 Standard (Mandatory) qualifiers: [-first] codon First codon usage file [-second] codon Second codon usage file for comparison [-outfile] outfile [*.codcmp] Output file name Additional (Optional) qualifiers: (none) Advanced (Unprompted) qualifiers: (none) Associated qualifiers: "-first" associated qualifiers -format1 string Data format "-second" associated qualifiers -format2 string Data format "-outfile" associated qualifiers -odirectory3 string Output directory General qualifiers: -auto boolean Turn off prompts -stdout boolean Write first file to standard output -filter boolean Read first file from standard input, write first file to 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 and exit. 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 -version boolean Report version number and exit Input file format It reads in the Codon Usage Tables - these are available as EMBOSS data files. See below for details. Output file format Output files for usage example File: eecoli.codcmp # CODCMP codon usage table comparison # Eecoli.cut vs Ehaein.cut Sum Squared Difference = 2.178 Mean Squared Difference = 0.034 Root Mean Squared Difference = 0.184 Sum Difference = 9.504 Mean Difference = 0.149 Codons not appearing = 0 Data files codcmp requires two codon usage tables which are read by default from the EMBOSS data file from Ehum.cut in the data/CODONS directory of the EMBOSS distribution. If the name of a codon usage file is specified on the command line, then this file will first be searched for in the current directory and then in the data/CODONS directory of the EMBOSS distribution. EMBOSS data files are distributed with the application and stored in the standard EMBOSS data directory, which is defined by the EMBOSS environment variable EMBOSS_DATA. To see the available EMBOSS data files, run: % embossdata -showall To fetch one of the data files (for example 'Exxx.dat') into your current directory for you to inspect or modify, run: % embossdata -fetch -file Exxx.dat Users can provide their own data files in their own directories. Project specific files can be put in the current directory, or for tidier directory listings in a subdirectory called ".embossdata". Files for all EMBOSS runs can be put in the user's home directory, or again in a subdirectory called ".embossdata". The directories are searched in the following order: * . (your current directory) * .embossdata (under your current directory) * ~/ (your home directory) * ~/.embossdata Notes The following notes based on Derek Gatherer's comments are useful for interpreting the significance of any difference between the tables. It's not normally possible to be certain a a difference is statistically significant just from looking at it, as it is essentially a descriptive statistic about the difference between two 64-mer vectors. If you have a whole lot of sequences and codcmp results for all the possible pairwise comparisons, then the resulting distance matrix can be used to build a phylogenetic tree based on codon usage. However, if you generate a series of random sequences, measure their codon usage and then do codcmp between each of your test sequences and all the random sequences, you could then use a z-test to see if the result between the two test sequences was outside of the top or bottom 5%. This would assume that the codcmp results were normally distributed, but you could test that too. The simplest way is just to plot them and look for a bell-curve. For more rigour, find the mean and standard deviation of your results from the random sequences, use the normal distribution equation to generate a theoretical distribution for that mean and standard deviation, and then perform a chi square between the random data and the theoretically generated normal distribution. If you generate two sets of random data, each based on your two test sequences, an F-test should be used to establish that they have equal variances. Then you can safely go ahead and perform the z-test. You could use the shuffle program to base your random sequences on the test sequences - so that would ensure the randomised background had the same nucleotide content. F-tests, z-tests and chi-tests can all be done in Excel, as well as being standard in most statistical analysis packages. References None. Warnings None. Diagnostic Error Messages None. Exit status This program always exits with a status of 0. Known bugs None. See also Program name Description cai Calculate codon adaptation index chips Calculates Nc codon usage statistic codcopy Copy and reformat a codon usage table cusp Create a codon usage table from nucleotide sequence(s) syco Draw synonymous codon usage statistic plot for a nucleotide sequence Author(s) Alan Bleasby European Bioinformatics Institute, Wellcome Trust Genome Campus, Hinxton, Cambridge CB10 1SD, UK Please report all bugs to the EMBOSS bug team (emboss-bug (c) emboss.open-bio.org) not to the original author. Some more statistics were added by David Martin Please report all bugs to the EMBOSS bug team (emboss-bug (c) emboss.open-bio.org) not to the original author. History Completed 9 Sept 1999 20 Oct 2000 - David Martin added a couple more statistics to the output. Target users This program is intended to be used by everyone and everything, from naive users to embedded scripts. Comments None