Last data update: Aug 15, 2025. (Total: 49733 publications since 2009)
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| Query Trace: Najdowski Morgan[original query] |
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| Effectiveness of nirsevimab among infants in their first RSV season in the United States, October 2023–March 2024: a test-negative design analysis
Payne Amanda B , Battan-Wraith Steph , Rowley Elizabeth AK , Stockwell Melissa S , Tartof Sara Y , Dascomb Kristin , Irving Stephanie A , Dixon Brian , Ball Sarah W , Tenforde Mark W , Vazquez-Benitez Gabriela , Stephens Ashley B , Han Jungmi , Natarajan Karthik , Salas SBianca , Bezi Cassandra , Sy Lina S , Lewin Bruno , Sheffield Tamara , Arndorfer Julie , Bride Daniel , Van Otterloo Josh , Naleway Allison L , Koppolu Padma D , Grannis Shaun , Fadel William , Rogerson Colin , Duszynski Tom , Reese Sarah E , Mitchell Patrick K , Chickery Sean , Moline Heidi L , Najdowski Morgan , Ciesla Allison Avrich , Reeves Emily L , DeSilva Malini , Fleming-Dutra Katherine E , Link-Gelles Ruth . Lancet Reg Health Am 2025 49 
Background: In August 2023, the Centers for Disease Control and Prevention recommended nirsevimab, a long-acting monoclonal antibody, for all U.S. infants aged <8 months entering or born during their first respiratory syncytial virus (RSV) season. Our aim was to estimate nirsevimab effectiveness against RSV-associated emergency department (ED) encounters and hospitalisation among U.S. infants during the 2023–2024 RSV season. Methods: We conducted a test-negative analysis using electronic health record (EHR) data from 6 healthcare systems, including ED encounters and hospitalizations with a diagnosis of RSV-like illness (RLI) during October 8, 2023–March 31, 2024, among infants aged <8 months as of October 1, 2023, or born during the study period. Nirsevimab effectiveness was estimated by comparing children who received nirsevimab with those who did not among RSV-positive and RSV-negative encounters, adjusting for age, race and ethnicity, sex, calendar day, and geographic region and excluding infants whose mother received RSV vaccination during pregnancy. Findings: Among 5039 ED encounters with RLI among infants in their first RSV season, 2045 (41%) were RSV-positive and 446 (9%) received nirsevimab, with a median time since dose of 52 days (interquartile range [IQR]: 27–84 days). Among 1025 hospitalizations with RLI among infants in their first RSV season, 605 (59%) were RSV-positive and 95 (9%) received nirsevimab, with a median time since dose of 48 days (IQR: 24–82 days). Nirsevimab effectiveness was 77% (95% CI: 69%–83%) against RSV-associated ED encounters and 98% (95% CI: 95%–99%) against RSV-associated hospitalisation. Interpretation: Nirsevimab was effective in preventing RSV-associated ED encounters and hospitalisation among infants in their first RSV season, with greatest protection against hospitalisation. However, these estimates reflect a short interval from nirsevimab administration to RLI onset. Since nirsevimab is a passive immunization and concentration is expected to wane over time, it is important to continue monitoring effectiveness to assess effectiveness with increased time since dose. Funding: This work was supported by the Centers for Disease Control and Prevention (contracts 75D30121D12779 to Westat and 75D30123C18039 to Kaiser Foundation Hospitals). © 2025 Elsevier B.V., All rights reserved. |
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