Experimental evolution and genome sequencing reveal variation in levels of clonal interference in large populations of bacteriophage φX174

<p>Abstract</p> <p>Background</p> <p>In large asexual populations where beneficial mutations may co-occur and recombination is absent, the fate of beneficial mutations can be significantly affected by competition (i.e., clonal interference). Theoretical models predict t...

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Main Authors: Pepin Kim M, Wichman Holly A
Format: Article
Language:English
Published: BMC 2008-03-01
Series:BMC Evolutionary Biology
Online Access:http://www.biomedcentral.com/1471-2148/8/85
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spelling doaj-311feba8f6ca442e8267befeb178afce2021-09-02T08:30:38ZengBMCBMC Evolutionary Biology1471-21482008-03-01818510.1186/1471-2148-8-85Experimental evolution and genome sequencing reveal variation in levels of clonal interference in large populations of bacteriophage φX174Pepin Kim MWichman Holly A<p>Abstract</p> <p>Background</p> <p>In large asexual populations where beneficial mutations may co-occur and recombination is absent, the fate of beneficial mutations can be significantly affected by competition (i.e., clonal interference). Theoretical models predict that clonal interference (CI) can slow adaptation, alter the distribution of fixed beneficial mutations, and affect disease progression by impacting within-host evolution of pathogens. While phenotypic data support that CI is a significant determinant of adaptive outcome, genetic data are needed to verify the patterns and to inform evolutionary models. We adapted replicate populations of the bacteriophage φX174 under two levels of CaCl<sub>2 </sub>to create benign and harsh environments. Genomic sequences of multiple individuals from evolved populations were used to detect competing beneficial mutations.</p> <p>Results</p> <p>There were several competing genotypes in most of the populations where CaCl<sub>2 </sub>was abundant, but no evidence of CI where CaCl<sub>2 </sub>was scarce, even though rates of adaptation and population sizes among the treatments were similar. The sequence data revealed that observed mutations were limited to a single portion of one gene in the harsh treatment, but spanned a different and larger region of the genome under the benign treatments, suggesting that there were more adaptive solutions to the benign treatment.</p> <p>Conclusion</p> <p>Beneficial mutations with relatively large selection coefficients can be excluded by CI. CI may commonly determine the fate of beneficial mutations in large microbial populations, but its occurrence depends on selective conditions. CI was more frequent in benign selective conditions possibly due to a greater number of adaptive targets under this treatment. Additionally, the genomic sequence data showed that selection can target different types and numbers of phenotypes in environments that differ by only a single continuous variable.</p> http://www.biomedcentral.com/1471-2148/8/85
collection DOAJ
language English
format Article
sources DOAJ
author Pepin Kim M
Wichman Holly A
spellingShingle Pepin Kim M
Wichman Holly A
Experimental evolution and genome sequencing reveal variation in levels of clonal interference in large populations of bacteriophage φX174
BMC Evolutionary Biology
author_facet Pepin Kim M
Wichman Holly A
author_sort Pepin Kim M
title Experimental evolution and genome sequencing reveal variation in levels of clonal interference in large populations of bacteriophage φX174
title_short Experimental evolution and genome sequencing reveal variation in levels of clonal interference in large populations of bacteriophage φX174
title_full Experimental evolution and genome sequencing reveal variation in levels of clonal interference in large populations of bacteriophage φX174
title_fullStr Experimental evolution and genome sequencing reveal variation in levels of clonal interference in large populations of bacteriophage φX174
title_full_unstemmed Experimental evolution and genome sequencing reveal variation in levels of clonal interference in large populations of bacteriophage φX174
title_sort experimental evolution and genome sequencing reveal variation in levels of clonal interference in large populations of bacteriophage φx174
publisher BMC
series BMC Evolutionary Biology
issn 1471-2148
publishDate 2008-03-01
description <p>Abstract</p> <p>Background</p> <p>In large asexual populations where beneficial mutations may co-occur and recombination is absent, the fate of beneficial mutations can be significantly affected by competition (i.e., clonal interference). Theoretical models predict that clonal interference (CI) can slow adaptation, alter the distribution of fixed beneficial mutations, and affect disease progression by impacting within-host evolution of pathogens. While phenotypic data support that CI is a significant determinant of adaptive outcome, genetic data are needed to verify the patterns and to inform evolutionary models. We adapted replicate populations of the bacteriophage φX174 under two levels of CaCl<sub>2 </sub>to create benign and harsh environments. Genomic sequences of multiple individuals from evolved populations were used to detect competing beneficial mutations.</p> <p>Results</p> <p>There were several competing genotypes in most of the populations where CaCl<sub>2 </sub>was abundant, but no evidence of CI where CaCl<sub>2 </sub>was scarce, even though rates of adaptation and population sizes among the treatments were similar. The sequence data revealed that observed mutations were limited to a single portion of one gene in the harsh treatment, but spanned a different and larger region of the genome under the benign treatments, suggesting that there were more adaptive solutions to the benign treatment.</p> <p>Conclusion</p> <p>Beneficial mutations with relatively large selection coefficients can be excluded by CI. CI may commonly determine the fate of beneficial mutations in large microbial populations, but its occurrence depends on selective conditions. CI was more frequent in benign selective conditions possibly due to a greater number of adaptive targets under this treatment. Additionally, the genomic sequence data showed that selection can target different types and numbers of phenotypes in environments that differ by only a single continuous variable.</p>
url http://www.biomedcentral.com/1471-2148/8/85
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