Issue: March 2019
January 04, 2019
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25% of sepsis cases following PCV13 introduction caused by S. pneumoniae

Issue: March 2019
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One-quarter of all community-acquired sepsis cases among Swiss children were attributable to Streptococcus pneumoniae shortly after the introduction of the 13-valent pneumococcal conjugate vaccine, or PCV13, according to research published in Clinical Infectious Diseases.

Perspective from Sheldon L. Kaplan, MD

The researchers wrote that despite the vaccine’s efficacy, infection caused by a vaccine serotype and pneumococcal meningitis were risk factors for more severe disease.

S. pneumoniae is a leading cause of sepsis, meningitis and community-acquired pneumonia, resulting in significant mortality in children worldwide,” Sandra A. Asner, MD, MSc, head of the pediatric infectious diseases unit and staff physician at Lausanne University Hospital, and colleagues wrote. “There is a lack of recent population-based studies determining the burden and outcomes of pneumococcal sepsis in children.”

Switzerland’s Federal Office of Public Health suggested that all children aged younger than 2 years should be vaccinated with PCV13 in 2011. The researchers examined rates of pneumococcal sepsis following the vaccine’s introduction. Between September 2011 and December 2015, children aged younger than 17 years with blood culture-confirmed pneumococcal sepsis who had systemic inflammatory response syndrome were prospectively recruited to the study.

“Importantly, our study was started in the first year of introduction of PCV13 into the general vaccine schedule in Switzerland,” the researchers wrote.

Asner and colleagues defined vaccine failure as infection caused by a vaccine serotype in a child who was up to date with all PCV doses.

The researchers detected 117 cases of pneumococcal sepsis and a crude incidence of two cases per 100,000 children (95% CI, 1.7-2.4). Pneumococcal sepsis accounted for 25% of all community-acquired sepsis episodes, they said, and the infection had an 8% case-fatality rate. Most children with pneumococcal sepsis (83%) were aged younger than 5 years and did not have known risk factors for invasive pneumococcal disease. Pediatric ICU admission was required for 36% of patients with pneumococcal sepsis.

Nonvaccine pneumococcal serotypes were responsible for most meningitis cases among children following the introduction of PCV13 (69% vs. 31%). Vaccine failure occurred in 26% of children, and 11 of these children were infected with serotype 3.

The researchers also observed an increased risk for pediatric ICU admission for children with pneumococcal meningitis (OR = 6.8; 95% CI, 2.4-19.3) or serotype 3 infection (OR = 2.8; 95% CI, 1.1-7.3). Additionally, children infected with serotype 3 — which is included in the vaccine — were more likely to have longer hospital stays.

Previous research examining the incidence of pneumococcal disease in the United Kingdom following PCV13 introduction was conducted at a time when vaccination rates for three doses was at 93.5%. Asner and colleagues speculated that herd immunity had not yet been achieved in their population because vaccine coverage with three doses of PCV13 was only between 75% and 80%.

“The inclusion of a large number of children who did not qualify for PCV vaccination because of their age (older than 5 years) were not or (younger than 5 months) not yet fully protected, or who did not follow the recommendations may account for this finding,” the researchers wrote. “Recent national surveillance data reported a 50% decrease in invasive pneumococcal disease among children aged younger than 5 years between 2009 and 2017 that may be increasing to 80% to 90% as seen in other countries, thus supporting the efficacy of PCV13 vaccination.”

The researchers noted, however, that the rate of infection with vaccine serotype 3 highlights the need for more effective vaccines and immunization schedules. – by Katherine Bortz

Disclosures: Asner reports no relevant financial disclosures. Please see the study for all other authors’ relevant financial disclosures.