Abstract
BACKGROUND: Following the introduction of routine administration of pneumococcal conjugate vaccines (PCV) to infants, more than half of children with invasive pneumococcal disease (IPD) in our surveillance study now have an underlying condition. We investigated IPD among children with and without underlying conditions to further characterize these groups. [Figure: see text] METHODS: Data from an ongoing U.S. pediatric multicenter pneumococcal surveillance study were analyzed from 2017-2023. We serotyped the isolates and collected patient characteristics including IPD presentation, age, underlying conditions and PCV history. Statistical analysis was performed using STATA version16. RESULTS: Among 660 cases with IPD, 210 had risk factors defined by the US Centers for Disease Control and Prevention (CDC) for the purpose of tailored vaccine directives and another 144 patients had other underlying conditions. (Table) Serotypes were available for 638 isolates. Differences among groups were observed for age, vaccine uptake, disease presentation and serotype distribution. Bacteremia was most common in patients with an immunocompromising condition and the most common serotype overall in this population was 23B (not contained in any licensed pediatric PCV). Serotypes 22F and 33F (both in PCV15 and PCV20) together caused 7% of cases; an additional 18% were of serotypes 10A, 11A, 12F and 15B (in PCV20). None of the unvaccinated patients in this group had a serotype 3 infection. Patients without underlying conditions were younger than the immune compromised, 50% presented with pneumonia or meningitis, and the most common serotype was 3. A higher percentage of children without CDC immunocompromising conditions presented with meningitis and mastoiditis. CONCLUSION: Our data show differences in clinical presentations and serotype distribution of IPD among children with or without known underlying conditions. PCV20 may provide additional protection for all groups and for the immunocompromised group, in particular, as 18% of their IPD isolates were serotypes not included in other licensed PCVs. Non-vaccine serotypes 15C, 23B, and 35B now are common causes of IPD in US children. DISCLOSURES: Kristina G. Hulten, PhD, Pfizer: Grant/Research Support William J. Barson, MD, Pfizer: Grant/Research Support Jennifer Dien Bard, PhD, D(ABMM), FIDSA, bioMerieux: Advisor/Consultant|bioMerieux: Grant/Research Support Lindsay Grant, PhD, MPH, Pfizer: Employee|Pfizer: Stocks/Bonds (Private Company) Adriano Arguedas, Medical director, Pfizer employee: employee|Pfizer employee: Stocks/Bonds (Public Company) Maria J. Tort, PhD, Pfizer, Inc: Stocks/Bonds (Public Company) Ashley Miller, MA, CCRP, Pfizer: Stocks/Bonds (Public Company) Alejandro D. Cane, MD, PhD, Pfizer Inc.: All authors are employees of Pfizer Inc. and may hold stock and/or stock options of Pfizer Inc. Sheldon L. Kaplan, MD, Pfizer: Grant/Research Support