Please use this identifier to cite or link to this item: http://hdl.handle.net/10400.7/873
Title: Recurrent Reverse Evolution Maintains Polymorphism after Strong Bottlenecks in Commensal Gut Bacteria
Author: Sousa, Ana
Ramiro, Ricardo S.
Barroso-Batista, João
Güleresi, Daniela
Lourenço, Marta
Gordo, Isabel
Keywords: experimental evolution
microbiota
reverse evolution
intrastrain polymorphism
nutritional optimization
precision medicine
Issue Date: Nov-2017
Publisher: Oxford University Press
Citation: Ana Sousa, Ricardo S. Ramiro, João Barroso-Batista, Daniela Güleresi, Marta Lourenço, Isabel Gordo; Recurrent Reverse Evolution Maintains Polymorphism after Strong Bottlenecks in Commensal Gut Bacteria, Molecular Biology and Evolution, Volume 34, Issue 11, 1 November 2017, Pages 2879–2892, https://doi.org/10.1093/molbev/msx221
Abstract: The evolution of new strains within the gut ecosystem is poorly understood. We used a natural but controlled system to follow the emergence of intraspecies diversity of commensal Escherichia coli, during three rounds of adaptation to the mouse gut (∼1,300 generations). We previously showed that, in the first round, a strongly beneficial phenotype (loss-of-function for galactitol consumption; gat-negative) spread to >90% frequency in all colonized mice. Here, we show that this loss-of-function is repeatedly reversed when a gat-negative clone colonizes new mice. The regain of function occurs via compensatory mutation and reversion, the latter leaving no trace of past adaptation. We further show that loss-of-function adaptive mutants reevolve, after colonization with an evolved gat-positive clone. Thus, even under strong bottlenecks a regime of strong-mutation-strong-selection dominates adaptation. Coupling experiments and modeling, we establish that reverse evolution recurrently generates two coexisting phenotypes within the microbiota that can or not consume galactitol (gat-positive and gat-negative, respectively). Although the abundance of the dominant strain, the gat-negative, depends on the microbiota composition, gat-positive abundance is independent of the microbiota composition and can be precisely manipulated by supplementing the diet with galactitol. These results show that a specific diet is able to change the abundance of specific strains. Importantly, we find polymorphism for these phenotypes in indigenous Enterobacteria of mice and man. Our results demonstrate that natural selection can greatly overwhelm genetic drift at structuring the strain diversity of gut commensals and that competition for limiting resources may be a key mechanism for maintaining polymorphism in the gut.
Description: The deposited article is a post-print version and has been submitted to peer review.
This deposit is composed by the main article plus the supplementary materials of the publication.
Peer review: yes
URI: http://hdl.handle.net/10400.7/873
DOI: 10.1093/molbev/msx221
Publisher Version: https://academic.oup.com/mbe/article/34/11/2879/4086164
Appears in Collections:EB - Articles

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