Localized Hypermutation is the Major Driver of Meningococcal Genetic Variability during Persistent Asymptomatic Carriage

Green, Luke R.; Al-Rubaiawi, Ali Abdulwahid Abed; Al-Maeni, Mohammad Abdul Rahmman; Harrison, Odile; Blades, Matthew; Oldfield, Neil J.; Turner, David P. J.; Maiden, Martin; Bayliss, Christopher

doi:10.1128/mbio.03068-19

Cited by 11 publications

(17 citation statements)

References 55 publications

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“…Mutation rates varied between 4.8 and 0.24 mutations/genome/month. These mutation accumulation rates are similar to those observed for longitudinal meningococcal carriage ( Lamelas et al, 2014 ; Pandey et al, 2018 ; Green et al, 2020 ), indicating that transmission does not impose a strong selection for elevated fixation of mutants or for higher mutability. Putative recombination fragments were found in almost all clusters at varying frequencies, with greater detection in the diverse phylogenetic clusters (i.e., A, F, and G) potentially reflecting divergence among founder clones.…”

Section: Discussionsupporting

confidence: 76%

“…For clusters with a single putative founder (i.e., B, C, D, and E), mutation and horizontal gene transfer generated similar numbers of variant genes (47 and 33, respectively) with an average of 20 variable genes per cluster. This latter rate is only 2.8-fold higher than occurs during persistent carriage in an individual (Green et al, 2020) and implies that rapid spread of meningococcal clones in a naïve population does not require significant levels of genetic variation.…”

Section: Discussionmentioning

confidence: 86%

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Rapid Transmission of a Hyper-Virulent Meningococcal Clone Due to High Effective Contact Numbers and Super Spreaders

et al. 2020

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Rapid transmission, a critical contributory factor in outbreaks of invasive meningococcal disease, requires naïve populations of sufficient size and intermingling. We examined genomic variability and transmission dynamics in a student population subject to an 11-fold increase in carriage of a hypervirulent Neisseria meningitidis serogroup W ST-11 clone. Phylogenetic clusters, mutation and recombination rates were derived by bioinformatic analyses of whole-genome sequencing data. Transmission dynamics were determined by combining observed carriage rates, cluster sizes and distributions with simple SIS models. Between 9 and 15 genetically-distinct clusters were detected and associated with seven residential halls. Clusters had low mutation accumulation rates and infrequent recombination events. Modeling indicated that effective contacts decreased from 10 to 2 per day between the start and mid-point of the university term. Transmission rates fluctuated between 1 and 4% while the R(t) for carriage decreased from an initial rate of 47 to 1. Decreases in transmission values correlated with a rise in vaccine-induced immunity. Observed carriage dynamics could be mimicked by populations containing 20% of super spreaders with 2.3-fold higher effective contact rates. We conclude that spread of this hypervirulent ST-11 meningococcal clone depends on the levels of effective contacts and immunity rather than genomic variability. Additionally, we propose that super-spreaders enhance meningococcal transmission and that a 70% MenACWY immunization level is sufficient to retard, but not fully prevent, meningococcal spread in close-contact populations.

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Section: Discussionsupporting

confidence: 76%

Section: Discussionmentioning

confidence: 86%

Rapid Transmission of a Hyper-Virulent Meningococcal Clone Due to High Effective Contact Numbers and Super Spreaders

et al. 2020

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“…Apart from porA (NEIS1364), a known non-functional orthologue of the gonococcal locus, none of the loci have known functions. NEIS0202 was identified as a hypermutable locus during persistent nasopharyngeal carriage [58], which may support the hypothesis for its involvement in colonization. Of the remaining genes with hypothetical functions, NEIS0332, encoding a type II toxinantitoxin, could be involved in initiating cell division while NEIS2056 may encode hemK, a peptide methyltransferase that controls translation termination [59].…”

Section: Loss-of-function In 24 Loci Is Associated With Cc53 But Not Hypervirulent Lineagessupporting

confidence: 68%

Modelling evolutionary pathways for commensalism and hypervirulence in Neisseria meningitidis

et al. 2021

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Neisseria meningitidis , the meningococcus, resides exclusively in humans and causes invasive meningococcal disease (IMD). The population of N. meningitidis is structured into stable clonal complexes by limited horizontal recombination in this naturally transformable species. N. meningitidis is an opportunistic pathogen, with some clonal complexes, such as cc53, effectively acting as commensal colonizers, while other genetic lineages, such as cc11, are rarely colonizers but are over-represented in IMD and are termed hypervirulent. This study examined theoretical evolutionary pathways for pathogenic and commensal lineages by examining the prevalence of horizontally acquired genomic islands (GIs) and loss-of-function (LOF) mutations. Using a collection of 4850 genomes from the BIGSdb database, we identified 82 GIs in the pan-genome of 11 lineages (10 hypervirulent and one commensal lineage). A new computational tool, Phaser, was used to identify frameshift mutations, which were examined for statistically significant association with genetic lineage. Phaser identified a total of 144 frameshift loci of which 105 were shown to have a statistically significant non-random distribution in phase status. The 82 GIs, but not the LOF loci, were associated with genetic lineage and invasiveness using the disease carriage ratio metric. These observations have been integrated into a new model that infers the early events of the evolution of the human adapted meningococcus. These pathways are enriched for GIs that are involved in modulating attachment to the host, growth rate, iron uptake and toxin expression which are proposed to increase competition within the meningococcal population for the limited environmental niche of the human nasopharynx. We surmise that competition for the host mucosal surface with the nasopharyngeal microbiome has led to the selection of isolates with traits that enable access to cell types (non-phagocytic and phagocytic) in the submucosal tissues leading to an increased risk for IMD.

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“…Previously published rates in carriage isolates are of the same order of magnitude to what we find in our study. Carriage isolates from the University of Nottingham had a mutation rate of 12.2 nucleotide substitutions per year [33]. In serogroup A carriage isolates from Africa, the mutation rate was 6.2 nucleotide substitutions per year [34].…”

Section: Discussionmentioning

confidence: 99%

Diversification in immunogenicity genes caused by selective pressures in invasive meningococci

et al. 2020

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We studied population genomics of 486 Neisseria meningitidis isolates causing meningitis in the Netherlands during the period 1979–2003 and 2006–2013 using whole-genome sequencing to evaluate the impact of a hyperendemic period of serogroup B invasive disease. The majority of serogroup B isolates belonged to ST-41/44 (41 %) and ST-32 complex (16 %). Comparing the time periods, before and after the decline of serogroup B invasive disease, there was a decrease of ST-41/44 complex sequences (P=0.002). We observed the expansion of a sub-lineage within ST-41/44 complex sequences being associated with isolation from the 1979–2003 time period (P=0.014). Isolates belonging to this sub-lineage expansion within ST-41/44 complex were marked by four antigen allele variants. Presence of these allele variants was associated with isolation from the 1979–2003 time period after correction for multiple testing (Wald test, P=0.0043 for FetA 1–5; P=0.0035 for FHbp 14; P=0.012 for PorA 7–2.4 and P=0.0031 for NHBA two peptide allele). These sequences were associated with 4CMenB vaccine coverage (Fisher’s exact test, P<0.001). Outside of the sub-lineage expansion, isolates with markedly lower levels of predicted vaccine coverage clustered in phylogenetic groups showing a trend towards isolation in the 2006–2013 time period (P=0.08). In conclusion, we show the emergence and decline of a sub-lineage expansion within ST-41/44 complex isolates concurrent with a hyperendemic period in meningococcal meningitis. The expansion was marked by specific antigen peptide allele combinations. We observed preliminary evidence for decreasing 4CMenB vaccine coverage in the post-hyperendemic period.

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Localized Hypermutation is the Major Driver of Meningococcal Genetic Variability during Persistent Asymptomatic Carriage

Cited by 11 publications

References 55 publications

Rapid Transmission of a Hyper-Virulent Meningococcal Clone Due to High Effective Contact Numbers and Super Spreaders

Rapid Transmission of a Hyper-Virulent Meningococcal Clone Due to High Effective Contact Numbers and Super Spreaders

Modelling evolutionary pathways for commensalism and hypervirulence in Neisseria meningitidis

Diversification in immunogenicity genes caused by selective pressures in invasive meningococci

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