Pervasive GxE interactions shape adaptive trajectories and the exploration of the phenotypic space in artificial selection experiments

Author:

Desbiez-Piat ArnaudORCID,Ressayre AdrienneORCID,Marchadier ElodieORCID,Noly Alicia,Remoué CarineORCID,Vitte ClémentineORCID,Belcram HarryORCID,Bourgais Aurélie,Galic Nathalie,Le Guilloux Martine,Tenaillon Maud I.ORCID,Dillmann ChristineORCID

Abstract

AbstractQuantitative genetics models have shown that long-term selection responses depend on initial variance and mutational influx. Understanding limits of selection requires quantifying the role of mutational variance. However, correlative responses to selection on non-focal traits can perturb the selection response on the focal trait; and generations are often confounded with selection environments so that genotype by environment (GxE) interactions are ignored. The Saclay Divergent Selection Experiments (DSE) on maize flowering time were used to track the fate of individual mutations combining genotyping data and phenotyping data from yearly measurements (DSEYM) and common garden experiments (DSECG) with four objectives (1) to quantify the relative contribution of standing and mutational variance to the selection response, (2) to estimate genotypic mutation effects, (3) to study the impact of GxE interactions in the selection response, (4) to analyze how trait correlations modulate the exploration of the phenotypic space. We validated experimentally the expected enrichment of fixed beneficial mutations with an average effect of +0.278 and +0.299 days to flowering, depending on the genetic background. Fixation of unfavorable mutations reached up to 25% of incoming mutations, a genetic load possibly due to antagonistic pleiotropy, whereby mutations fixed in the selection environment (DSEYM) turned to be unfavorable in the evaluation environment (DSECG). Global patterns of trait correlations were conserved across genetic backgrounds but exhibited temporal patterns. Traits weakly or uncorrelated with flowering time triggered stochastic exploration of the phenotypic space, owing to microenvironment-specific fixation of standing variants and pleiotropic mutational input.

Publisher

Cold Spring Harbor Laboratory

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