The Implications of Lineage-Specific Rates for Divergence Time Estimation
Author(s) -
Tom Carruthers,
Michael J. Sanderson,
Robert W. Scotland
Publication year - 2019
Publication title -
systematic biology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 7.128
H-Index - 182
eISSN - 1076-836X
pISSN - 1063-5157
DOI - 10.1093/sysbio/syz080
Subject(s) - biology , divergence (linguistics) , lineage (genetic) , locus (genetics) , evolutionary biology , statistics , bayesian probability , bayes' theorem , rate of evolution , residual , genetics , gene , mathematics , phylogenetics , algorithm , philosophy , linguistics
Rate variation adds considerable complexity to divergence time estimation in molecular phylogenies. Here, we evaluate the impact of lineage-specific rates —which we define as among-branch-rate-variation that acts consistently across the entire genome. We compare its impact to residual rates —defined as among-branch-rate-variation that shows a different pattern of rate variation at each sampled locus, and gene-specific rates —defined as variation in the average rate across all branches at each sampled locus. We show that lineage-specific rates lead to erroneous divergence time estimates, regardless of how many loci are sampled. Further, we show that stronger lineage-specific rates lead to increasing error. This contrasts to residual rates and gene-specific rates, where sampling more loci significantly reduces error. If divergence times are inferred in a Bayesian framework, we highlight that error caused by lineage-specific rates significantly reduces the probability that the 95% highest posterior density includes the correct value, and leads to sensitivity to the prior. Use of a more complex rate prior—which has recently been proposed to model rate variation more accurately—does not affect these conclusions. Finally, we show that the scale of lineage-specific rates used in our simulation experiments is comparable to that of an empirical data set for the angiosperm genus Ipomoea . Taken together, our findings demonstrate that lineage-specific rates cause error in divergence time estimates, and that this error is not overcome by analyzing genomic scale multilocus data sets. [Divergence time estimation; error; rate variation.]
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