Abstract

BackgroundSince 2009, increases in the incidence of invasive meningococcal disease have occurred in the United Kingdom due to a sublineage of the Neisseria meningitidis serogroup W ST-11 clonal complex (hereafter, the “original UK strain”). In 2013, a descendent substrain (hereafter, the “2013 strain”) became the dominant disease-causing variant. Multiple outer-membrane proteins of meningococci are subject to phase-variable switches in expression due to hypermutable simple-sequence repeats. We investigated whether alterations in phase-variable genes may have influenced the relative prevalence of the original UK and 2013 substrains, using multiple disease and carriage isolates.MethodsRepeat numbers were determined by either bioinformatics analysis of whole-genome sequencing data or polymerase chain reaction amplification and sizing of fragments from genomic DNA extracts. Immunoblotting and sequence-translation analysis was performed to identify expression states.ResultsSignificant increases in repeat numbers were detected between the original UK and 2013 strains in genes encoding PorA, NadA, and 2 Opa variants. Invasive and carriage isolates exhibited similar repeat numbers, but the absence of pilC gene expression was frequently associated with disease.ConclusionsElevated repeat numbers in outer-membrane protein genes of the 2013 strain are indicative of higher phase-variation rates, suggesting that rapid expansion of this strain was due to a heightened ability to evade host immune responses during transmission and asymptomatic carriage.

Highlights

  • Since 2009, increases in invasive meningococcal disease have occurred in the United Kingdom due to a sub-lineage of the Neisseria meningitidis serogroup W ST-11 clonal complex

  • While changes t in simple sequence repeats (SSR) during persistent asymptomatic carriage can lead to a reduction in expression of outer membrane proteins (OMP) [15], ip there has been no extensive comparison of SSRs or PV states between carriage and invasive isolates r of a single clonal complex. sc This study compares the repeat numbers and expression states of phase-variable OMPs for the u MenW ST-11 lineage between: i) the original-UK and 2013- strains; ii) carriage and invasive isolates. n We demonstrate a heightened potential for PV of multiple OMPs in the 2013-strain and reduced a expression of PilC proteins in invasive isolates

  • Allelic variation in phase-variable scOMP of ST-11 MenW carriage and invasive isolates We assessed the association of PV with IMD by focusing on the UK cc11 MenW strains using 636 UK invasive disease isolates and 101 UK carriage isolates (i.e. 47 and t 54 isolates obtained from university students in a 2010-2011 longitudinal or 2015-2016 crossip sectional study, respectively)

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Summary

Introduction

Since 2009, increases in invasive meningococcal disease have occurred in the United Kingdom due to a sub-lineage of the Neisseria meningitidis serogroup W ST-11 clonal complex (the ‘original-UK’ strain). Sc This study compares the repeat numbers and expression states of phase-variable OMPs for the u MenW ST-11 lineage between: i) the original-UK and 2013- strains; ii) carriage and invasive isolates. Repeat numbers in seven phase-variable scOMPs and the two pilC loci were determined for >93% of 737 MenW ST-11 isolates (Supplementary Data File 1).

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Conclusion
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