The molecular clock of neutral evolution can be accelerated or slowed by asymmetric spatial structure.
Over time, a population acquires neutral genetic substitutions as a consequence of random drift. A famous result in population genetics asserts that the rate, K, at which these substitutions accumulate in the population coincides with the mutation rate, u, at which they arise in individuals: K = u....
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doaj-2d46b26bd10243a28361cac22287c94d2020-11-25T01:33:53ZengPublic Library of Science (PLoS)PLoS Computational Biology1553-734X1553-73582015-02-01112e100410810.1371/journal.pcbi.1004108The molecular clock of neutral evolution can be accelerated or slowed by asymmetric spatial structure.Benjamin AllenChristine SampleYulia DementievaRuben C MedeirosChristopher PaolettiMartin A NowakOver time, a population acquires neutral genetic substitutions as a consequence of random drift. A famous result in population genetics asserts that the rate, K, at which these substitutions accumulate in the population coincides with the mutation rate, u, at which they arise in individuals: K = u. This identity enables genetic sequence data to be used as a "molecular clock" to estimate the timing of evolutionary events. While the molecular clock is known to be perturbed by selection, it is thought that K = u holds very generally for neutral evolution. Here we show that asymmetric spatial population structure can alter the molecular clock rate for neutral mutations, leading to either K<u or K>u. Our results apply to a general class of haploid, asexually reproducing, spatially structured populations. Deviations from K = u occur because mutations arise unequally at different sites and have different probabilities of fixation depending on where they arise. If birth rates are uniform across sites, then K ≤ u. In general, K can take any value between 0 and Nu. Our model can be applied to a variety of population structures. In one example, we investigate the accumulation of genetic mutations in the small intestine. In another application, we analyze over 900 Twitter networks to study the effect of network topology on the fixation of neutral innovations in social evolution.http://europepmc.org/articles/PMC4342344?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Benjamin Allen Christine Sample Yulia Dementieva Ruben C Medeiros Christopher Paoletti Martin A Nowak |
spellingShingle |
Benjamin Allen Christine Sample Yulia Dementieva Ruben C Medeiros Christopher Paoletti Martin A Nowak The molecular clock of neutral evolution can be accelerated or slowed by asymmetric spatial structure. PLoS Computational Biology |
author_facet |
Benjamin Allen Christine Sample Yulia Dementieva Ruben C Medeiros Christopher Paoletti Martin A Nowak |
author_sort |
Benjamin Allen |
title |
The molecular clock of neutral evolution can be accelerated or slowed by asymmetric spatial structure. |
title_short |
The molecular clock of neutral evolution can be accelerated or slowed by asymmetric spatial structure. |
title_full |
The molecular clock of neutral evolution can be accelerated or slowed by asymmetric spatial structure. |
title_fullStr |
The molecular clock of neutral evolution can be accelerated or slowed by asymmetric spatial structure. |
title_full_unstemmed |
The molecular clock of neutral evolution can be accelerated or slowed by asymmetric spatial structure. |
title_sort |
molecular clock of neutral evolution can be accelerated or slowed by asymmetric spatial structure. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS Computational Biology |
issn |
1553-734X 1553-7358 |
publishDate |
2015-02-01 |
description |
Over time, a population acquires neutral genetic substitutions as a consequence of random drift. A famous result in population genetics asserts that the rate, K, at which these substitutions accumulate in the population coincides with the mutation rate, u, at which they arise in individuals: K = u. This identity enables genetic sequence data to be used as a "molecular clock" to estimate the timing of evolutionary events. While the molecular clock is known to be perturbed by selection, it is thought that K = u holds very generally for neutral evolution. Here we show that asymmetric spatial population structure can alter the molecular clock rate for neutral mutations, leading to either K<u or K>u. Our results apply to a general class of haploid, asexually reproducing, spatially structured populations. Deviations from K = u occur because mutations arise unequally at different sites and have different probabilities of fixation depending on where they arise. If birth rates are uniform across sites, then K ≤ u. In general, K can take any value between 0 and Nu. Our model can be applied to a variety of population structures. In one example, we investigate the accumulation of genetic mutations in the small intestine. In another application, we analyze over 900 Twitter networks to study the effect of network topology on the fixation of neutral innovations in social evolution. |
url |
http://europepmc.org/articles/PMC4342344?pdf=render |
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