Publications by authors named "Josh Hamilton"
Epidemiological studies report the impact of co-infection with pneumococcus and respiratory viruses upon disease rates and outcomes, but their effect on pneumococcal carriage acquisition and bacterial load is scarcely described. Here, we assess this by combining natural viral infection with controlled human pneumococcal infection in 581 healthy adults screened for upper respiratory tract viral infection before intranasal pneumococcal challenge. Across all adults, respiratory syncytial virus (RSV) and rhinovirus asymptomatic infection confer a substantial increase in secondary infection with pneumococcus.
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- Respiratory mucosal immunity from vaccination is essential for protection against coronavirus, but its effectiveness in humans, especially after a prior SARS-CoV-2 infection, is unclear.
- Research shows that individuals who have been both infected and vaccinated have higher levels of SARS-CoV-2 antibodies and B cells in their airways compared to those who were only vaccinated.
- Infection leads to the development of specific memory T cells in the lungs that persist longer than those generated by vaccination alone, indicating a need for vaccines designed to target airway immunity.
serotype 3 (SPN3) is a cause of invasive pneumococcal disease and associated with low carriage rates. Following the introduction of pediatric 13-valent pneumococcal conjugate vaccine (PCV13) programs, SPN3 declines are less than other vaccine serotypes and incidence has increased in some populations coincident with a shift in predominant circulating SPN3 clade, from I to II. A human challenge model provides an effective means for assessing the impact of PCV13 on SPN3 in the upper airway.
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