Use of an individual-based model of pneumococcal carriage for planning a randomized trial of a whole-cell vaccine
Authored by Marc Lipsitch, Francisco Y Cai, Thomas Fussell, Sarah Cobey
Date Published: 2018
DOI: 10.1371/journal.pcbi.1006333
Sponsors:
No sponsors listed
Platforms:
C++
Model Documentation:
Other Narrative
Model Code URLs:
https://github.com/ocsicnarf/vaccine-trial-planning
Abstract
For encapsulated bacteria such as Streptococcus pneumoniae, asymptomatic
carriage is more common and longer in duration than disease, and hence
is often a more convenient endpoint for clinical trials of vaccines
against these bacteria. However, using a carriage endpoint entails
specific challenges. Carriage is almost always measured as prevalence,
whereas the vaccine may act by reducing incidence or duration. Thus, to
determine sample size requirements, its impact on prevalence must first
be estimated. The relationship between incidence and prevalence (or
duration and prevalence) is convex, saturating at 100\% prevalence. For
this reason, the proportional effect of a vaccine on prevalence is
typically less than its proportional effect on incidence or duration.
This relationship is further complicated in the presence of multiple
pathogen strains. In addition, host immunity to carriage accumulates
rapidly with frequent exposures in early years of life, creating
potentially complex interactions with the vaccine's effect. We conducted
a simulation study to predict the impact of an inactivated whole cell
pneumococcal vaccine-believed to reduce carriage duration-on carriage
prevalence in different age groups and trial settings. We used an
individual-based model of pneumococcal carriage that incorporates
relevant immunological processes, both vaccine-induced and naturally
acquired. Our simulations showed that for a wide range of vaccine
efficacies, sampling time and age at vaccination are important
determinants of sample size. There is a window of favorable sampling
times during which the required sample size is relatively low, and this
window is prolonged with a younger age at vaccination, and in a trial
setting with lower transmission intensity. These results illustrate the
ability of simulation studies to inform the planning of vaccine trials
with carriage endpoints, and the methods we present here can be applied
to trials evaluating other pneumococcal vaccine candidates or comparing
alternative dosing schedules for the existing conjugate vaccines.
Tags
Design
Children
Efficacy
Colonization
Conjugate vaccine
Streptococcus-pneumoniae
Nasopharyngeal carriage
Epidemiologic evidence
Acquired-immunity