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Comparative Study
. 2002;3(2):RESEARCH0008.
doi: 10.1186/gb-2002-3-2-research0008. Epub 2002 Jan 14.

Selection in the evolution of gene duplications

Affiliations
Comparative Study

Selection in the evolution of gene duplications

Fyodor A Kondrashov et al. Genome Biol. 2002.

Abstract

Background: Gene duplications have a major role in the evolution of new biological functions. Theoretical studies often assume that a duplication per se is selectively neutral and that, following a duplication, one of the gene copies is freed from purifying (stabilizing) selection, which creates the potential for evolution of a new function.

Results: In search of systematic evidence of accelerated evolution after duplication, we used data from 26 bacterial, six archaeal, and seven eukaryotic genomes to compare the mode and strength of selection acting on recently duplicated genes (paralogs) and on similarly diverged, unduplicated orthologous genes in different species. We find that the ratio of nonsynonymous to synonymous substitutions (Kn/Ks) in most paralogous pairs is <<1 and that paralogs typically evolve at similar rates, without significant asymmetry, indicating that both paralogs produced by a duplication are subject to purifying selection. This selection is, however, substantially weaker than the purifying selection affecting unduplicated orthologs that have diverged to the same extent as the analyzed paralogs. Most of the recently duplicated genes appear to be involved in various forms of environmental response; in particular, many of them encode membrane and secreted proteins.

Conclusions: The results of this analysis indicate that recently duplicated paralogs evolve faster than orthologs with the same level of divergence and similar functions, but apparently do not experience a phase of neutral evolution. We hypothesize that gene duplications that persist in an evolving lineage are beneficial from the time of their origin, due primarily to a protein dosage effect in response to variable environmental conditions; duplications are likely to give rise to new functions at a later phase of their evolution once a higher level of divergence is reached.

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Figures

Figure 1
Figure 1
Synonymous and nonsynonymous substitution rates for (a,b) paralogs and (c,d) orthologs from (a,c) bacteria and (b,d) mammals. All points with Ks > 0.5 (approaching saturation) were assigned a Ks value of 0.5. In (b), the blue circles represent human duplicated genes and the red circles show duplicated genes from mouse and rat. In (d), the blue circles are human-rodent orthologous comparisons, and the red circles are the mouse-rat comparisons.

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