Within-host Mycobacterium tuberculosis evolution: a population genetics perspective

ABSTRACTThe within-host evolutionary dynamics of TB remain unclear, and underlying biological characteristics render standard population genetic approaches based upon the Wright-Fisher model largely inappropriate. In addition, the compact genome combined with an absence of recombination is expected to result in strong purifying selection effects. Thus, it is imperative to establish a biologically-relevant evolutionary framework incorporating these factors in order to enable an accurate study of this important human pathogen. Further, such a model is critical for inferring fundamental evolutionary parameters related to patient treatment, including mutation rates and the severity of infection bottlenecks. We here implement such a model and infer the underlying evolutionary parameters governing within-patient evolutionary dynamics. Results demonstrate that the progeny skew associated with the clonal nature of TB severely reduces genetic diversity and that the neglect of this parameter in previous studies has led to significant mis-inference of mutation rates. As such, our results suggest an underlying de novo mutation rate that is considerably faster than previously inferred, and a progeny distribution differing significantly from Wright-Fisher assumptions. This inference largely reconciles the seemingly contradictory observations of both rapid drug-resistance evolution but extremely low levels of genetic variation in both resistant and non-resistant populations.

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Evolutionary dynamics of bacteria in the gut microbiome within and across hosts

10.1101/210955 ◽

2017 ◽

Cited By ~ 10

Author(s):

Nandita R. Garud ◽

Benjamin H. Good ◽

Oskar Hallatschek ◽

Katherine S. Pollard

Keyword(s):

Evolutionary Dynamics ◽

Purifying Selection ◽

Gut Bacteria ◽

Fundamental Limits ◽

Evolutionary Forces ◽

Standard Population ◽

Evolutionary Changes ◽

Or Gene ◽

Adult Twins ◽

Long Timescales

AbstractGut microbiota are shaped by a combination of ecological and evolutionary forces. While the ecological dynamics have been extensively studied, much less is known about how species of gut bacteria evolve over time. Here we introduce a model-based framework for quantifying evolutionary dynamics within and across hosts using a panel of metagenomic samples. We use this approach to study evolution in ∼30 prevalent species in the human gut. Although the patterns of between-host diversity are consistent with quasi-sexual evolution and purifying selection on long timescales, we identify new genealogical signatures that challenge standard population genetic models of these processes. Within hosts, we find that genetic differences that accumulate over ∼6 month timescales are only rarely attributable to replacement by distantly related strains. Instead, the resident strains more commonly acquire a smaller number of putative evolutionary changes, in which nucleotide variants or gene gains or losses rapidly sweep to high frequency. By comparing these mutations with the typical between-host differences, we find evidence that some sweeps are seeded by recombination, in addition to new mutations. However, comparisons of adult twins suggest that replacement eventually overwhelms evolution over multi-decade timescales, hinting at fundamental limits to the extent of local adaptation. Together, our results suggest that gut bacteria can evolve on human-relevant timescales, and they highlight the connections between these short-term evolutionary dynamics and longer-term evolution across hosts.

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Within-host evolutionary dynamics of seasonal and pandemic human influenza A viruses in young children

eLife ◽

10.7554/elife.68917 ◽

2021 ◽

Vol 10 ◽

Author(s):

Alvin X Han ◽

Zandra C Felix Garza ◽

Matthijs RA Welkers ◽

René M Vigeveno ◽

Nhu Duong Tran ◽

...

Keyword(s):

Young Children ◽

Influenza A ◽

Evolutionary Dynamics ◽

De Novo ◽

Purifying Selection ◽

Influenza Viruses ◽

Human Influenza ◽

Influenza A Viruses ◽

Virus Diversity ◽

Host Evolution

The evolution of influenza viruses is fundamentally shaped by within-host processes. However, the within-host evolutionary dynamics of influenza viruses remain incompletely understood, in part because most studies have focused on infections in healthy adults based on single timepoint data. Here, we analysed the within-host evolution of 82 longitudinally-sampled individuals, mostly young children, infected with A/H1N1pdm09 or A/H3N2 viruses between 2007 and 2009. For A/H1N1pdm09 infections during the 2009 pandemic, nonsynonymous minority variants were more prevalent than synonymous ones. For A/H3N2 viruses in young children, early infection was dominated by purifying selection. As these infections progressed, nonsynonymous variants typically increased in frequency even when within-host virus titres decreased. Unlike the short-lived infections of adults where de novo within-host variants are rare, longer infections in young children allow for the maintenance of virus diversity via mutation-selection balance creating potentially important opportunities for within-host virus evolution.

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A Global Analysis of Mutations Accompanying Microevolution in the Heterozygous Diploid Pathogen Candida albicans

10.1101/288597 ◽

2018 ◽

Author(s):

Iuliana V. Ene ◽

Rhys A. Farrer ◽

Matthew P. Hirakawa ◽

Kennedy Agwamba ◽

Christina A. Cuomo ◽

...

Keyword(s):

Candida Albicans ◽

Large Scale ◽

De Novo ◽

Global Analysis ◽

Purifying Selection ◽

Opportunistic Pathogen ◽

Mutation Rates ◽

Colonization Model ◽

Chromosomal Changes ◽

Host Infection

AbstractCandida albicans is a heterozygous diploid yeast that is a commensal of the human gastrointestinal (GI) tract and a prevalent opportunistic pathogen. Here, whole-genome sequencing was performed on multiple C. albicans isolates passaged in different niches to characterize the complete spectrum of mutations arising during microevolution. We reveal that evolution during short time-scales (<600 generations) is driven by both de novo base substitutions and short-tract loss of heterozygosity (LOH) events. In contrast, large-scale chromosomal changes are relatively rare, although chromosome 7 trisomies repeatedly emerged during passaging in one GI colonization model. Both strain background and chromosomal features affected mutational patterns, with mutation rates being greatly elevated in regions adjacent to emergent LOH tracts. Mutation rates were also elevated during host infection where genomes showed strong evidence of purifying selection. These results establish the genetic events driving C. albicans evolution and that this heterozygous diploid is extensively shaped by purifying selection.

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De novo structural mutation rates and gamete-of-origin biases revealed through genome sequencing of 2,396 families

The American Journal of Human Genetics ◽

10.1016/j.ajhg.2021.02.012 ◽

2021 ◽

Author(s):

Jonathan R. Belyeu ◽

Harrison Brand ◽

Harold Wang ◽

Xuefang Zhao ◽

Brent S. Pedersen ◽

...

Keyword(s):

Genome Sequencing ◽

De Novo ◽

Mutation Rates ◽

Structural Mutation

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Purifying Selection, Drift, and Reversible Mutation with Arbitrarily High Mutation Rates

Genetics ◽

10.1534/genetics.114.167973 ◽

2014 ◽

Vol 198 (4) ◽

pp. 1587-1602 ◽

Cited By ~ 30

Author(s):

Brian Charlesworth ◽

Kavita Jain

Keyword(s):

Purifying Selection ◽

Mutation Rates ◽

Reversible Mutation

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EVOLUTION WITH ENDOGENOUS MUTATIONS

International Game Theory Review ◽

10.1142/s0219198905000508 ◽

2005 ◽

Vol 07 (02) ◽

pp. 229-240 ◽

Cited By ~ 1

Author(s):

IVAR KOLSTAD

Keyword(s):

Evolutionary Dynamics ◽

Basin Of Attraction ◽

Equilibrium Selection ◽

Mutation Rates ◽

And Control

Bergin and Lipman (1996) prove that equilibrium selection in the evolutionary dynamics of Kandori et al. (1993) and Young (1993), is not robust to variations in mutation rates across states. Specifically, a risk dominant equilibrium can be selected against if mutation rates are higher in its basin of attraction than elsewhere. Van Damme and Weibull (1998) model mutations as a compromise between payoff losses and control costs, which implies lower mutation rates in the risk dominant equilibrium. This paper argues that this result is not driven by control costs, but by players focusing on payoff losses when choosing mutation rates.

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Transfer RNA genes experience exceptionally elevated mutation rates

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.1801240115 ◽

2018 ◽

Vol 115 (36) ◽

pp. 8996-9001 ◽

Cited By ~ 12

Author(s):

Bryan P. Thornlow ◽

Josh Hough ◽

Jacquelyn M. Roger ◽

Henry Gong ◽

Todd M. Lowe ◽

...

Keyword(s):

Mutation Rate ◽

Trna Gene ◽

Gene Evolution ◽

Purifying Selection ◽

Mutation Rates ◽

Model Organisms ◽

Biological Synthesis ◽

Human Populations ◽

Trna Genes ◽

Simple Method

Transfer RNAs (tRNAs) are a central component for the biological synthesis of proteins, and they are among the most highly conserved and frequently transcribed genes in all living things. Despite their clear significance for fundamental cellular processes, the forces governing tRNA evolution are poorly understood. We present evidence that transcription-associated mutagenesis and strong purifying selection are key determinants of patterns of sequence variation within and surrounding tRNA genes in humans and diverse model organisms. Remarkably, the mutation rate at broadly expressed cytosolic tRNA loci is likely between 7 and 10 times greater than the nuclear genome average. Furthermore, evolutionary analyses provide strong evidence that tRNA genes, but not their flanking sequences, experience strong purifying selection acting against this elevated mutation rate. We also find a strong correlation between tRNA expression levels and the mutation rates in their immediate flanking regions, suggesting a simple method for estimating individual tRNA gene activity. Collectively, this study illuminates the extreme competing forces in tRNA gene evolution and indicates that mutations at tRNA loci contribute disproportionately to mutational load and have unexplored fitness consequences in human populations.

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Diversity and evolution of surface polysaccharide synthesis loci in Enterobacteriales

10.1101/709832 ◽

2019 ◽

Author(s):

Kathryn E. Holt ◽

Florent Lassalle ◽

Kelly L. Wyres ◽

Ryan Wick ◽

Rafal J. Mostowy

Keyword(s):

Evolutionary Dynamics ◽

Bacterial Species ◽

Purifying Selection ◽

Evolutionary Forces ◽

Polysaccharide Synthesis ◽

Surface Polysaccharides ◽

Surface Polysaccharide ◽

Selective Preservation ◽

Multiple Species

Bacterial capsules and lipopolysaccharides are diverse surface polysaccharides (SPs) that serve as the frontline for interactions with the outside world. While SPs can evolve rapidly, their diversity and evolutionary dynamics across different taxonomic scales has not been investigated in detail. Here, we focused on the bacterial order Enterobacteriales (including the medically-relevant Enterobacteriaceae), to carry out comparative genomics of two SP locus synthesis regions, cps and kps, using 27,334 genomes from 45 genera. We identified high-quality cps loci in 22 genera and kps in 11 genera, around 4% of which were detected in multiple species. We found SP loci to be highly dynamic genetic entities: their evolution was driven by high rates of horizontal gene transfer (HGT), both of whole loci and component genes, and relaxed purifying selection, yielding large repertoires of SP diversity. In spite of that, we found the presence of (near-)identical locus structures in distant taxonomic backgrounds that could not be explained by recent exchange, pointing to long-term selective preservation of locus structures in some populations. Our results reveal differences in evolutionary dynamics driving SP diversity within different bacterial species, with lineages of Escherichia coli, Enterobacter hormachei and Klebsiella aerogenes most likely to share SP loci via recent exchange; and lineages of Salmonella enterica, Citrobacter sakazakii and Serratia marcescens most likely to share SP loci via other mechanisms such as long-term preservation. Overall, the evolution of SP loci in Enterobacteriales is driven by a range of evolutionary forces and their dynamics and relative importance varies between different species.

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Red queen's race: rapid evolutionary dynamics of an expanding family of meiotic drive factors and their hpRNA suppressors

10.1101/2021.08.05.454923 ◽

2021 ◽

Author(s):

Jeffrey Vedanayagam ◽

Ching-Jung Lin ◽

Eric C. Lai

Keyword(s):

Evolutionary Dynamics ◽

Sex Chromosome ◽

De Novo ◽

Independent Set ◽

Meiotic Drive ◽

Sperm Chromatin ◽

Arms Races ◽

X Chromosomes ◽

Selfish Genetic Elements ◽

Satellite Repeats

Meiotic drivers are a class of selfish genetic elements that are widespread across eukaryotes. Their activities are often detrimental to organismal fitness and thus trigger drive suppression to ensure fair segregation during meiosis. Accordingly, their existence is frequently hidden in genomes, and their molecular functions are little known. Here, we trace evolutionary steps that generated the Dox meiotic drive system in Drosophila simulans (Dsim), which distorts male:female balance (sex-ratio) by depleting male progeny. We show that Dox emerged via stepwise mobilization and acquisition of portions of multiple D. melanogaster genes, including the sperm chromatin packaging gene protamine. Moreover, we reveal novel Dox homologs in Dsim and massive, recent, amplification of Dox superfamily genes specifically on X chromosomes of its closest sister species D. mauritiana (Dmau) and D. sechellia (Dsech). The emergence of Dox superfamily genes is tightly associated with 1.688 family satellite repeats that flank de novo genomic copies. In concert, we find coordinated emergence and diversification of autosomal hairpin RNA/siRNAs loci that target subsets of Dox superfamily genes across simulans clade species. Finally, an independent set of protamine amplifications the Y chromosome of D. melanogaster indicates that protamine genes are frequent and recurrent players in sex chromosome dynamics. Overall, we reveal fierce genetic arms races between meiotic drive factors and siRNA suppressors associated with recent speciation.

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Sequence diversity and evolution of an iflavirus family associated with ticks

10.1101/2020.06.02.129551 ◽

2020 ◽

Author(s):

Romain Daveu ◽

Caroline Hervet ◽

Louane Sigrist ◽

Davide Sassera ◽

Aaron Jex ◽

...

Keyword(s):

Cell Line ◽

Complete Genome ◽

Evolutionary Dynamics ◽

De Novo ◽

Rna Viruses ◽

Ixodes Scapularis ◽

Fine Scale ◽

Rna Seq ◽

Strong Positive Selection ◽

Synonymous Mutations

AbstractWe studied a family of iflaviruses, a group of RNA viruses frequently found in arthropods, focusing on viruses associated with ticks. Our aim was to bring insight on the evolutionary dynamics of this group of viruses, which may interact with the biology of ticks. We explored systematically de novo RNA-Seq assemblies available for species of ticks which allowed to identify nine new genomes of iflaviruses. The phylogeny of virus sequences was not congruent with that of the tick hosts, suggesting recurrent host changes across tick genera along evolution. We identified five different variants with a complete or near-complete genome in Ixodes ricinus. These sequences were closely related, which allowed a fine-scale estimation of patterns of substitutions: we detected a strong excess of synonymous mutations suggesting evolution under strong positive selection. ISIV, a sequence found in the ISE6 cell line of Ixodes scapularis, was unexpectedly nearidentical with I. ricinus variants, suggesting a contamination of this cell line by I. ricinus material. Overall, our work constitutes a step in the understanding of the interactions between this family of viruses and ticks.

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