4.8 Article

Historical Contingency Drives Compensatory Evolution and Rare Reversal of Phage Resistance

期刊

MOLECULAR BIOLOGY AND EVOLUTION
卷 39, 期 9, 页码 -

出版社

OXFORD UNIV PRESS
DOI: 10.1093/molbev/msac182

关键词

historical contingency; epistasis; experimental evolution; parallel evolution; bacteriophages; microbial evolution

资金

  1. National Science Foundation [1650114, 1942881]
  2. Society for the Study of Evolution [047408]
  3. Amgen Foundation (Amgen Scholars Fellowship)
  4. Direct For Biological Sciences
  5. Division Of Integrative Organismal Systems [1942881] Funding Source: National Science Foundation

向作者/读者索取更多资源

Bacteria and lytic viruses (phages) have a coevolutionary relationship, and this study explores how phages shape the future evolutionary trajectories of their host populations. The researchers found that some bacteria populations re-evolved phage sensitivity over time, while others acquired compensatory mutations that reduced the costs of resistance. The genetic mechanisms of resistance and the initial evolution of resistance played a significant role in these outcomes. This study highlights the importance of phages in the ecological and evolutionary dynamics of their host communities and provides insights into the genetic architecture of historical contingency.
Bacteria and lytic viruses (phages) engage in highly dynamic coevolutionary interactions over time, yet we have little idea of how transient selection by phages might shape the future evolutionary trajectories of their host populations. To explore this question, we generated genetically diverse phage-resistant mutants of the bacterium Pseudomonas syringae. We subjected the panel of mutants to prolonged experimental evolution in the absence of phages. Some populations re-evolved phage sensitivity, whereas others acquired compensatory mutations that reduced the costs of resistance without altering resistance levels. To ask whether these outcomes were driven by the initial genetic mechanisms of resistance, we next evolved independent replicates of each individual mutant in the absence of phages. We found a strong signature of historical contingency: some mutations were highly reversible across replicate populations, whereas others were highly entrenched. Through whole-genome sequencing of bacteria over time, we also found that populations with the same resistance gene acquired more parallel sets of mutations than populations with different resistance genes, suggesting that compensatory adaptation is also contingent on how resistance initially evolved. Our study identifies an evolutionary ratchet in bacteria-phage coevolution and may explain previous observations that resistance persists over time in some bacterial populations but is lost in others. We add to a growing body of work describing the key role of phages in the ecological and evolutionary dynamics of their host communities. Beyond this specific trait, our study provides a new insight into the genetic architecture of historical contingency, a crucial component of interpreting and predicting evolution.

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