Dear Miguel,
> I noted that phylogenetic trees reconstructed from a protein dataset
> under (1) a single partition that includes all the sites of the dataset
> or under (2) a partition per site (whatever is -brlen) based on the same
> exchangeability matrix, differ in terms of both topology and branch
> lenghts.
That might happen if you change the model.
> It seems that using a partition for every site
Are you really using a separate partition for every single site?
That might induce substantial over-parametrization.
> instead of a
> partition for all the sites (both under the same exchangeability matrix)
> dramatically reduces the accuracy of the reconstructed phylogenetic
> tree, is it correct?.
You might be over-parametrizing, to provide a more detailed answer I
would need to know the alignment size (#taxa and #sites) and you should
send me your partition file.
> Is there any way to reconstruct the same (or very
> similar) phylogenetic tree with/without partitions under the same
> exchangeability matrix?
I think that there is no clear answer to this, the general rule is: if
you change the model under which you infer the tree you get might change
as well. You may want to consider running PartitionFinder or analogous
tools to find an appropriate partition scheme.
Alexis
> Thank you!
> Best,
> Miguel
>
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--
Alexandros (Alexis) Stamatakis
ERA Chair, Institute of Computer Science, Foundation for Research and
Technology - Hellas
Research Group Leader, Heidelberg Institute for Theoretical Studies
Full Professor, Dept. of Informatics, Karlsruhe Institute of Technology
www.biocomp.gr (Crete lab)
www.exelixis-lab.org (Heidelberg lab)