Mutational biases favor complexity increases in protein interaction networks after gene duplication

Author:

Cisneros Angel FORCID,Nielly-Thibault Lou,Mallik Saurav,Levy Emmanuel D,Landry Christian RORCID

Abstract

AbstractBiological systems can gain complexity over time. While some of these transitions are likely driven by natural selection, the extent to which they occur without providing an adaptive benefit is unknown. At the molecular level, one example is heteromeric complexes replacing homomeric ones following gene duplication. Here, we build a biophysical model and simulate the evolution of homodimers and heterodimers following gene duplication using distributions of mutational effects inferred from available protein structures. We keep the specific activity of each dimer identical, so their concentrations drift neutrally without new functions. We show that for more than 60% of tested dimer structures, the relative concentration of the heteromer increases over time due to mutational biases that favor the heterodimer. However, allowing mutational effects on synthesis rates and differences in the specific activity of homo- and heterodimers can limit or reverse the observed bias toward heterodimers. Our results show that the accumulation of more complex protein quaternary structures is likely under neutral evolution, and that natural selection would be needed to reverse this tendency.

Funder

Canadian Government | Canadian Institutes of Health Research

Canada Research Chair in Cellular and Systems Biology

FRQ | Fonds de recherche du Québec – Nature et technologies

Agencia Mexicana de Cooperación Internacional para el Desarrollo

Mitacs

Canadian Government | Natural Sciences and Engineering Research Council of Canada

EC | ERC | HORIZON EUROPE European Research Council

Israel Science Foundation

Abisch-Frenkel Foundation

Publisher

Springer Science and Business Media LLC

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