Abstract
Bacteria generally live in species-rich communities, such as the gut microbiota. Yet little is known about bacterial evolution in natural ecosystems. Here, we followed the long-term evolution of commensal Escherichia coli in the mouse gut. We observe the emergence of mutation rate polymorphism, ranging from wild-type levels to 1,000-fold higher. By combining experiments, whole-genome sequencing, and in silico simulations, we identify the molecular causes and explore the evolutionary conditions allowing these hypermutators to emerge and coexist within the microbiota. The hypermutator phenotype is caused by mutations in DNA polymerase III proofreading and catalytic subunits, which increase mutation rate by approximately 1,000-fold and stabilise hypermutator fitness, respectively. Strong mutation rate variation persists for >1,000 generations, with coexistence between lineages carrying 4 to >600 mutations. The in vivo molecular evolution pattern is consistent with fitness effects of deleterious mutations sd ≤ 10−4/generation, assuming a constant effect or exponentially distributed effects with a constant mean. Such effects are lower than typical in vitro estimates, leading to a low mutational load, an inference that is observed in in vivo and in vitro competitions. Despite large numbers of deleterious mutations, we identify multiple beneficial mutations that do not reach fixation over long periods of time. This indicates that the dynamics of beneficial mutations are not shaped by constant positive Darwinian selection but could be explained by other evolutionary mechanisms that maintain genetic diversity. Thus, microbial evolution in the gut is likely characterised by partial sweeps of beneficial mutations combined with hitchhiking of slightly deleterious mutations, which take a long time to be purged because they impose a low mutational load. The combination of these two processes could allow for the long-term maintenance of intraspecies genetic diversity, including mutation rate polymorphism. These results are consistent with the pattern of genetic polymorphism that is emerging from metagenomics studies of the human gut microbiota, suggesting that we have identified key evolutionary processes shaping the genetic composition of this community.
Highlights
Bacteria typically live in multispecies ecosystems [1]
Emergence and maintenance of mutation rate variation in a gut commensal strain To be able to study the evolution of new E. coli strains as they invade and colonise the mouse gut, we used a short-course antibiotic treatment (8 days with streptomycin), which perturbs microbiota composition and leads to a decrease in its species diversity
Given the observed mutation rate increase of about 1,000-fold for clones isolated from mice and that it is possible for mutation rate variation to emerge during the engineering process, we suggest that the DnaQL145P single mutant (dnaQ) mutation is responsible for the approximately 1,000-fold mutation rate increase
Summary
Bacteria typically live in multispecies ecosystems [1]. One of such communities is the human gut microbiota, which is key for host health and can host up to 1013 bacteria and hundreds of species. It has become clear that there can be abundant genetic diversity within each species colonising a given individual [5,6,7,8]. Strain level variation is key for multiple phenotypes ranging from antibiotic resistance and virulence to colonisation resistance (e.g., [9,10,11]). Little is known about how different evolutionary mechanisms—such as mutation, recombination, migration, genetic drift, and natural selection—shape bacterial genetic diversity within the mammalian gut [12]
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