The impact of aggregating serogroups in dynamic models of Neisseria meningitidis transmission
Authored by Chris T Bauch, Keith D Poore
Date Published: 2015
DOI: 10.1186/s12879-015-1015-8
Sponsors:
National Science and Engineering Research Council of Canada (NSERC)
Platforms:
No platforms listed
Model Documentation:
Other Narrative
Model Code URLs:
Model code not found
Abstract
Background: Neisseria meningitidis (Nm) is a pathogen of multiple
serogroups that is highly prevalent in many populations. Serogroups
associated with invasive meningococcal disease (IMD) in Canada, for
example, include A, B, C, W-135, X and Y. IMD is a rare but serious
outcome of Nm infection, and can be prevented with vaccines that target
certain serogroups. This has stimulated the development of dynamic
models to evaluate vaccine impact. However, these models typically
aggregate the various Nm serogroups into a small number of combined
groups, instead of modelling each serogroup individually. The impact of
aggregation on dynamic Nm model predictions is poorly understood. Our
objective was to explore the impact of aggregation on dynamic model
predictions.
Methods: We developed two age-structured agent-based models-a 2-strain
model and a 4-strain model-to simulate vaccination programs in the
Canadian setting. The 2-strain model was used to explore two different
groupings: C, versus all other serogroups combined; and B, versus all
other serogroups combined. The 4-strain model used the four groupings:
C, B, Neisseria lactamica, versus all other serogroups combined. We
compared the predicted impact of monovalent C vaccine, quadrivalent ACWY
vaccine (MCV-4), and monovalent B vaccine (4CMenB) on the prevalence of
serogroup carriage under these different models.
Results: The 2-strain and 4-strain models predicted similar overall
impacts of vaccines on carriage prevalence, especially with respect to
the vaccine-targeted serogroups. However, there were some significant
quantitative and qualitative differences. Declines in vaccine-targeted
serogroups were more rapid in the 2-strain model than the 4-strain
model, for both the C and the 4CMenB vaccines. Sustained oscillations, and evidence for multiple attractors (i.e., different types of dynamics
for the same model parameters but different initial conditions), occurred in the 4-strain model but not the 2-strain model. Strain
replacement was also more pronounced in the 4-strain model, on account
of the 4-strain model spreading prevalence more thinly across groups and
thus enhancing competitive interactions.
Conclusions: Simplifying assumptions like aggregation of serogroups can
have significant impacts on dynamic model predictions. Modellers should
carefully weigh the advantages and disadvantages of aggregation when
formulating models for multi-strain pathogens.
Tags
Epidemiology
Influenza
Outbreaks
C conjugate vaccination
Outer-membrane proteins
Meningococcal disease
Carriage
Lactamica
Immunity
Induction