Author:
Tan Susanna K.,Granados Andrea C.,Bouquet Jerome,Hoy-Schulz Yana Emmy,Green Lauri,Federman Scot,Stryke Doug,Haggerty Thomas D.,Ley Catherine,Yeh Ming-Te,Jannat Kaniz,Maldonado Yvonne A.,Andino Raul,Parsonnet Julie,Chiu Charles Y.
Abstract
AbstractThe potential role of enteric viral infections and the developing infant virome in affecting immune responses to the oral poliovirus vaccine (OPV) is unknown. Here we performed viral metagenomic sequencing on 3 serially collected stool samples from 30 Bangladeshi infants following OPV vaccination and compared findings to stool samples from 16 age-matched infants in the United States (US). In 14 Bangladeshi infants, available post-vaccination serum samples were tested for polio-neutralizing antibodies. The abundance (p = 0.006) and richness (p = 0.013) of the eukaryotic virome increased with age and were higher than seen in age-matched US infants (p < 0.001). In contrast, phage diversity metrics remained stable and were similar to those in US infants. Non-poliovirus eukaryotic virus abundance (3.68 log10 vs. 2.25 log10, p = 0.002), particularly from potential viral pathogens (2.78log10 vs. 0.83log10, p = 0.002), and richness (p = 0.016) were inversely associated with poliovirus shedding. Following vaccination, 28.6% of 14 infants tested developed neutralizing antibodies to all three Sabin types and also exhibited higher rates of poliovirus shedding (p = 0.020). No vaccine-derived poliovirus variants were detected. These results reveal an inverse association between eukaryotic virome abundance and poliovirus shedding. Overall gut virome ecology and concurrent viral infections may impact oral vaccine responsiveness in Bangladeshi infants.
Funder
National Institutes of Health,United States
Bill and Melinda Gates Foundation
Thrasher Research Fund
Global Health Equity Scholars Program
Lucile Packard Foundation for Children's Health
Stanford University
National Institutes of Health
Publisher
Springer Science and Business Media LLC
Cited by
6 articles.
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