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Complex Models
layout: userdoc title: "Complex Models" author: AUTHOR date: DATE docid: 11 icon: book doctype: manual tags:
- manual description: Complex models such as partition and mixture models. sections:
- name: Partition models url: partition-models
- name: Mixture models url: mixture-models
- name: Site-specific frequency models url: site-specific-frequency-models
- name: Heterotachy models url: heterotachy-models
Complex models such as partition and mixture models.
This document gives detailed descriptions of complex maximum-likelihood models available in IQ-TREE. It is assumed that you know the basic substitution models already.
Partition models are intended for phylogenomic (e.g., multi-gene) alignments, which allow each partition to have its own substitution models and evolutionary rates. IQ-TREE supports three types of partition models:
- Edge-equal partition model with equal branch lengths: All partitions share the same set of branch lengths.
- Edge-proportional partition model with proportional branch lengths: Like above but each partition has its own partition specific rate, that rescales all its branch lengths. This model accomodates different evolutionary rates between partitions (e.g. between 1st, 2nd, and 3rd codon positions).
- Edge-unlinked partition model: Each partition has its own set of branch lengths. This is the most parameter-rich partition model, that accounts for e.g., heterotachy (Lopez et al., 2002).
TIP: The edge-equal partition model is typically unrealistic as it does not account for different evolutionary speeds between partitions, whereas the edge-unlinked partition model can be overfitting if there are many short partitions. Therefore, the edge-proportional partition model is recommended for a typical analysis. {: .tip}
To apply partition models users must first prepare a partition file in RAxML-style or NEXUS format. The RAxML-style is defined by the RAxML software and may look like:
DNA, part1 = 1-100
DNA, part2 = 101-384
This means two DNA partitions of an alignment, where one groups aligment sites 1-100
into part1
and 101-384
into part2
.
The NEXUS format is more complex but more powerful. For example, the above partition scheme may look like:
#nexus
begin sets;
charset part1 = 1-100;
charset part2 = 101-384;
charpartition mine = HKY+G:part1, GTR+I+G:part2;
end;
The first line contains the keyword #nexus
to indicate a NEXUS file. It has a sets
block, which contains two character sets (charset
command) named part1
and part2
. Furthermore, with the charpartition
command we set the model HKY+G
for part1
and GTR+I+G
for part2
. This is not possible with the RAxML-style format (i.e., one cannot specify +G
rate model for one partition and +I+G
rate model for the other partition).
TIP: IQ-TREE fully supports mixed rate heterogeneity types types between partitions (see above example). {: .tip}
One can also specify non-consecutive sites of a partition, e.g. under RAxML-style format:
DNA, part1 = 1-100, 250-384
DNA, part2 = 101-249\3, 102-249\3
DNA, part3 = 103-249\3
or under NEXUS format:
#nexus
begin sets;
charset part1 = 1-100 250-384;
charset part2 = 101-249\3 102-249\3;
charset part3 = 103-249\3;
end;
This means, part2
contains sites 101, 102, 104, 105, 107, ..., 246, 248, 249; whereas part3
contains sites 103, 106, ..., 247. This is useful to specify partitions corresponding to 1st, 2nd and 3rd codon positions.
Moreover, the NEXUS file allows each partition to come from a separate alignment file (not possible under RAxML-style format) with e.g.:
#nexus
begin sets;
charset part1 = aln1.phy: 1-100\3 201-300;
charset part2 = aln1.phy: 101-200;
charset part3 = aln2.phy: *;
charpartition mine = HKY:part1, GTR+G:part2, WAG+I+G:part3;
end;
Here, part1
and part2
correspond to sub-alignments of aln1.phy
file and part3
is the entire alignment file aln2.phy
. Note that aln2.phy
is a protein alignment in this example.
TIP: IQ-TREE fully supports mixed data types between partitions. {: .tip}
If you want to specify codon model for a partition, use the CODON
keyword (otherwise, the partition may be detected as DNA):
#nexus
begin sets;
charset part1 = aln1.phy:CODON, 1-300;
charset part2 = aln1.phy: 301-400;
charset part3 = aln2.phy: *;
charpartition mine = GY:part1, GTR+G:part2, WAG+I+G:part3;
end;
Note that this assumes part1
has standard genetic code. If not, append CODON
with the right genetic code ID.
Having prepared a partition file, one is ready to start a partitioned analysis with -q
(edge-equal), -spp
(edge-proportional) or -sp
(edge-unlinked) option. See this tutorial for more details.
Mixture models, like partition models, allow more than one substitution model along the sequences. However, while a partition model assigns each alignment site a given specific model, mixture models do not need this information: it will compute for each site its probability of belonging to each of the mixture classes (also called categories or components). Since the site-to-class assignment is not known, the site likelihood under mixture models is the weighted sum of site likelihoods per mixture class.
For example, the discrete Gamma rate heterogeneity is a simple type of mixture model, which have several rate categories with equal probability. IQ-TREE also supports a number of predefined protein mixture models such as the profile mixture models C10
to C60
(The ML variants of Bayesian CAT
models).
Here, we discuss several possibilities to define new mixture models in IQ-TREE.
To start with, the following command:
iqtree -s example.phy -m "MIX{JC,HKY}"
is a valid analysis. Here, we specify a mixture model (via MIX
keyword in the model string) with two components (JC
and HKY
model) given in curly bracket and comma separator. IQ-TREE will then estimate the parameters of both mixture components as well as their weights: the proportion of sites belonging to each component.
NOTE: Do not forget the double-quotes around model string! Otherwise, the Terminal/Console might not recognize the model string properly.
Mixture models can be combined with rate heterogeneity, e.g.:
iqtree -s example.phy -m "MIX{JC,HKY}+G4"
Here, we specify two models and four Gamma rate categories. Effectively it means that there are 8 mixture components! Each site has a probability belonging to either JC
or HKY
and to one of the four rate categories.
Sometimes one only wants to model the changes in nucleotide or amino-acid frequencies along the sequences while keeping the substitution rate matrix the same. This can be specified in IQ-TREE via FMIX{...}
model syntax. For convenience the mixture components can be defined in a NEXUS file like this (example corresponds to the CF4 model of (Wang et al., 2008)):
#nexus
begin models;
frequency Fclass1 = 0.02549352 0.01296012 0.005545202 0.006005566 0.01002193 0.01112289 0.008811948 0.001796161 0.004312188 0.2108274 0.2730413 0.01335451 0.07862202 0.03859909 0.005058205 0.008209453 0.03210019 0.002668138 0.01379098 0.2376598;
frequency Fclass2 = 0.09596966 0.008786096 0.02805857 0.01880183 0.005026264 0.006454635 0.01582725 0.7215719 0.003379354 0.002257725 0.003013483 0.01343441 0.001511657 0.002107865 0.006751404 0.04798539 0.01141559 0.000523736 0.002188483 0.004934972;
frequency Fclass3 = 0.01726065 0.005467988 0.01092937 0.3627871 0.001046402 0.01984758 0.5149206 0.004145081 0.002563289 0.002955213 0.005286931 0.01558693 0.002693098 0.002075771 0.003006167 0.01263069 0.01082144 0.000253451 0.001144787 0.004573568;
frequency Fclass4 = 0.1263139 0.09564027 0.07050061 0.03316681 0.02095119 0.05473468 0.02790523 0.009007538 0.03441334 0.005855319 0.008061884 0.1078084 0.009019514 0.05018693 0.07948 0.09447839 0.09258897 0.01390669 0.05367769 0.01230413;
frequency CF4model = FMIX{empirical,Fclass1,Fclass2,Fclass3,Fclass4};
end;
Here, the NEXUS file contains a models
block to define new models. More explicitly, we define four AA profiles Fclass1
to Fclass4
(each containing 20 AA frequencies). Then, the frequency mixture is defined with
FMIX{empirical,Fclass1,Fclass2,Fclass3,Fclass4}
That means, we have five components: the first corresponds to empirical AA frequencies to be inferred from the data and the remaining four components are specified in this NEXUS file. Please save this to a file, say, mymodels.nex
. One can now start the analysis with:
iqtree -s some_protein.aln -mdef mymodels.nex -m JTT+CF4model+G
The -mdef
option specifies the NEXUS file containing user-defined models. Here, the JTT
matrix is applied for all alignment sites and one varies the AA profiles along the alignment. One can use the NEXUS syntax to define all other profile mixture models such as C10
to C60
.
In fact, IQ-TREE uses this NEXUS model file internally to define all protein mixture models. In addition to defining state frequencies, one can specify the entire model with rate matrix and state frequencies together. For example, the LG4M model (Le et al., 2012) can be defined by:
#nexus
begin models;
model LG4M1 =
0.269343
0.254612 0.150988
0.236821 0.031863 0.659648
....;
....
model LG4M4 = ....;
model LG4M = MIX{LG4M1,LG4M2,LG4M3,LG4M4}*G4;
end;
Here, we first define the four matrices LG4M1
, LG4M2
, LG4M3
and LG4M4
in PAML format (see protein models). Then LG4M
is defined as mixture model with these four components fused with Gamma rate heterogeneity (via *G4
syntax instead of +G4
). This means that, in total, we have 4 mixture components instead of 16. The first component LG4M1
is rescaled by the rate of the lowest Gamma rate category. The fourth component LG4M4
corresponds to the highest rate.
Note that both frequency
and model
commands can be embedded into a single model file.
Starting with version 1.5.0, IQ-TREE provides a new posterior mean site frequency (PMSF) model as a rapid approximation to the time and memory consuming profile mixture models C10
to C60
(Le et al., 2008a; a variant of PhyloBayes' CAT
model). The PMSF are the amino-acid profiles for each alignment site computed from an input mixture model and a guide tree. The PMSF model is much faster and requires much less RAM than C10
to C60
(see table below), regardless of the number of mixture classes. Our extensive simulations and empirical phylogenomic data analyses demonstrate that the PMSF models can effectively ameliorate long branch attraction artefacts.
If you use this model in a publication please cite:
H.C. Wang, B.Q. Minh, S. Susko and A.J. Roger (2017) Modeling site heterogeneity with posterior mean site frequency profiles accelerates accurate phylogenomic estimation. Syst. Biol., in press. https://doi.org/10.1093/sysbio/syx068
Here is an example of computation time and RAM usage for an Obazoa data set (68 sequences, 43615 amino-acid sites) from Brown et al. (2013) using 16 CPU cores:
Models | CPU time | Wall-clock time | RAM usage |
---|---|---|---|
LG+F+G |
43h:38m:23s | 3h:37m:23s | 1.8 GB |
LG+C20+F+G |
584h:25m:29s | 46h:39m:06s | 38.8 GB |
LG+C60+F+G |
1502h:25m:31s | 125h:15m:29s | 112.8 GB |
LG+PMSF+G |
73h:30m:37s | 5h:7m:27s | 2.2 GB |
To use the PMSF model you have to provide a guide tree, which, for example, can be obtained by a quicker analysis under the simpler LG+F+G
model. The guide tree can then be specified via -ft
option, for example:
iqtree -s <alignment> -m LG+C20+F+G -ft <guide_tree>
Here, IQ-TREE will perform two phases. In the first phase, IQ-TREE estimates mixture model parameters given the guide tree and then infers the site-specific frequency profile (printed to .sitefreq
file). In the second phase, IQ-TREE will conduct typical analysis using the inferred frequency model instead of the mixture model to save RAM and running time. Note that without -ft
option, IQ-TREE will conduct the analysis under the specified mixture model.
The PMSF model allows one, for the first time, to conduct nonparametric bootstrap under such complex models, for example (with 100 bootstrap replicates):
iqtree -s <alignment> -m LG+C20+F+G -ft <guide_tree> -b 100
Please note that the first phase still consumes as much RAM as the mixture model. To overcome this, you can perform the first phase in a high-memory server and the second phase in a normal PC as follows:
iqtree -s <alignment> -m LG+C20+F+G -ft <guide_tree> -n 0
This will stop the analysis after the first phase and also write a .sitefreq
file. You can now copy this .sitefreq
file to another low-memory machine and run with the same alignment:
iqtree -s <alignment> -m LG+C20+F+G -fs <file.sitefreq> -b 100
This will omit the first phase and thus need much less RAM.
Finally, note that for long (phylogenomic) alignments you can utilize the multicore IQ-TREE version to further save the computing times with, say, 24 cores by:
iqtree-omp -nt 24 -s <alignment> -m LG+C20+F+G -fs <file.sitefreq>
See also the list of relevant command line options.
Sequence data that have evolved under heterotachy, i.e., rate variation across sites and lineages (Lopez, Casane, and Philippe, 2002), are known to mislead phylogenetic inference (Kolaczkowski and Thornton, 2004). To address this issue we introduce the General Heterogeneous evolution On a Single Topology (GHOST) model. More specifically, GHOST is an edge-unlinked mixture model consisting of several site classes, each having a separate set of model parameters and edge lengths on the same tree topology. Thus, GHOST naturally accounts for heterotachous evolution. In contrast to an edge-unlinked partition model, the GHOST model does not require the a priori data partitioning, a possible source of model misspecification.
Extensive simulations show that the GHOST model can accurately recover the tree topology, branch lengths, substitution rate and base frequency parameters from heterotachously-evolved sequences. Moreover, we compare the GHOST model to the partition model and show that, owing to the minimization of model constraints, the GHOST model is able to offer unique biological insights when applied to empirical data.
If you use this model in a publication please cite:
S.M. Crotty, B.Q. Minh, N.G. Bean, B.R. Holland, J. Tuke, L.S. Jermiin and A. von Haeseler (2017) GHOST: Recovering historical signal from heterotachously-evolved sequence alignments.
https://doi.org/10.1101/174789
Make sure that you have IQ-TREE version 1.6.0 or later. The GHOST model with k
mixture classes is executed by adding +Hk
to the model option (-m
). For example if one wants to fit a GHOST model with 4 classes in conjunction with the GTR
model of DNA evolution to sequences contained in data.fst
, one would use the following command:
iqtree -s data.fst -m GTR+H4
By default the above command will link GTR parameters across all classes. If you want to unlink GTR parameters, so that IQ-TREE estimates them separately for each class, replace +H4
by *H4
:
iqtree -s data.fst -m GTR*H4
Note that this infers one set of empirical base frequencies and apply those to all classes. If one wishes to infer separate base frequencies for each class then the +FO
option is required:
iqtree -s data.fst -m GTR+FO*H4
The -wspm
option will generate a .siteprob
output file. This contains the probability of each site belonging to each class:
iqtree -s data.fst -m GTR+FO*H4 -wspm
Copyright (c) 2010-2016 IQ-TREE development team.
- First example
- Model selection
- New model selection
- Codon models
- Binary, Morphological, SNPs
- Ultrafast bootstrap
- Nonparametric bootstrap
- Single branch tests
- Partitioned analysis
- Partitioning with mixed data
- Partition scheme selection
- Bootstrapping partition model
- Utilizing multi-core CPUs
- Tree topology tests
- User-defined models
- Consensus construction and bootstrap value assignment
- Computing Robinson-Foulds distance
- Generating random trees
- DNA models
- Protein models
- Codon models
- Binary, morphological models
- Ascertainment bias correction
- Rate heterogeneity
- Counts files
- First running example
- Substitution models
- Virtual population size
- Sampling method
- Bootstrap branch support
- Interpretation of branch lengths