ANGSD: Analysis of next generation Sequencing Data
Latest tar.gz version is (0.938/0.939 on github), see Change_log for changes, and download it here.
Allele Frequencies
The allele frequency is the relative frequency of an allele across all alleles for a site.
This can be polarized according to the major/minor, reference/non-refernce or ancestral/derived. Therefore the choice of allele frequency estimator is closely related to choosing which alleles are segregating (see Inferring_Major_and_Minor_alleles).
We allow for frequency estimation from different input data:
- Genotype Likelihoods
- Genotype posteriors
- Counts of bases
The allele frequency estimator from genotype likelihoods are from this publication, and the base counts method is from this publication. Unless you have very specific reasons for using the count based estimator we recommend that uses use the -doMaf 2.
Brief Overview
./angsd -doMaf -> angsd version: 0.570 build(Dec 17 2013 14:11:25) -> Analysis helpbox/synopsis information: ------------------------ analysisMaf.cpp: -doMaf 0 1: BFGS frequency (known major minor) 2: EM frequency (known major minor) 4: BFGS frequency (unknown major minor) 8: EM frequency (unknown major minor) 16: Frequency from genotype probabilities 32: AlleleCounts based method (known major minor) -doSNP 0 -minMaf 0.010000 0 -minLRT 24.000000 0 -ref (null) -anc (null) -eps 0.001000 [Only used for -doMaf &32] -doPost 0 (Calculate posterior prob 3xgprob) 1: Using frequency as prior 2: Using uniform prior -beagleProb 0 (Dump beagle style postprobs) NB these frequency estimators requires major/minor -doMajorMinor
Allele Frequency estimation
- -doMaf [int]
INT=1 bfgs known minor
INT=2 EM known minor
INT=4 BFGS unknown minor
INT=8 EM unknown minor
INT=16 frequencies from genotype probabilities
Multiple estimators can be used simultaniusly be summing up the above numbers. Thus -doMaf 7 (1+2+4) will use the first three estimators. If the allele frequencies are estimated from the genotype likelihoods then you need to infer the major and minor allele (-doMajorMinor)
Allele frequencies from genotype likelihoods
The allele frequency estimators are described in citation. For testing reasons two optimazations are availeble. The BFGS and the EM algorithm. The EM algorithm is much faster then the BFGS. The allele frequencies are estimated by assuming that the site is diallelic and the major or minor alleles can be infered prior to the estimation or the uncertaincy of the minor allele can be incorborated into the model.
Example
Example for estimating the allele frequencies both while assuming known major and minor allele but also while taking the uncertaincy of the minor allele inference into account. The inference of the major and minor allele is done directly from the genotype likelihood
./angsd -out out -doMajorMinor 1 -doMaf 10 -bam bam.filelist
Estimator from genotype probabilities
If the genotype probabilities are known the frequencies can be estimated by summing up the posterior probabilities where is the sequencing data and the allele count of the minor allele. The frequency estimate
example
Example of the use of a genotype probability file for example from the output from beagle.
./angsd -out out -doMaf 16 -beagle beagle.file.gz
Estimator from sequencing data
The allele frequencies can be infered directy from the sequencing data citation. This works by using "counts" of alleles, and should be invoked like
- -doCounts 1 -doPhat 1
Output data
.mafs
chromo position major minor ref knownEM unknownEM nInd 21 9719788 T A 0.000001 -0.000012 3 21 9719789 G A 0.000000 -0.000001 3 21 9719790 A C 0.000000 -0.000004 3 21 9719791 G A 0.000000 -0.000001 3 21 9719792 G A 0.000000 -0.000002 3 21 9719793 G T 0.498277 41.932766 3 21 9719794 T A 0.000000 -0.000001 3 21 9719795 T A 0.000000 -0.000001 3
The first 4 columns are always defined to be:
- 1. chromosome name
- 2. position
- 3. major allele
- 4. minor allele
Depending on whether or not a reference and/or ancestral fasta files has been supplied these can occur as column 5 and 6. There are 4 different MAF estimators the estimate for these are given by the names knownEM,unknownEM,knownBFGS,unknownBFGS.
Futhermore if -doSNP is included, then the corresponding LRT will be printed.
The nInd column is the effective sample size, as detmined by the genotype likelihoods.
Anders check below:
This pretty explanatory, nInd is the number of individuals where we have "reliable" reads (see bugs section)
Depending on -doMaf INT, and -ref FILENAME and -anc FILENAME, extra column will be input.