Pathogen kinetics and detection by next-generation sequencing in pediatric complicated pneumonia

Pediatric pneumonia can be severe and result in empyema. Next-generation sequencing (NGS) may broadly detect pathogens though, optimal timing and impact of sample type on diagnostic yield is unknown. This is a prospective, single-center pilot study of children aged 3 months through 17 years admitted...

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Veröffentlicht in:Diagnostic microbiology and infectious disease 2024-10, Vol.110 (2), p.116468, Article 116468
Hauptverfasser: Rodriguez, Katherine M., Perofsky, Katherine L., Ramchandar, Nanda, Foley, Jennifer, Shah, Nidhi, Mangifesta, Marta, Schlaberg, Robert, Farnaes, Lauge, Stinnett, Rita Czako, Coufal, Nicole G.
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Sprache:eng
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Zusammenfassung:Pediatric pneumonia can be severe and result in empyema. Next-generation sequencing (NGS) may broadly detect pathogens though, optimal timing and impact of sample type on diagnostic yield is unknown. This is a prospective, single-center pilot study of children aged 3 months through 17 years admitted to the PICU with a primary diagnosis of complicated pneumonia. Plasma, endotracheal, nasopharyngeal, and pleural fluid samples were collected at three time points during hospitalization. After nucleic acid extraction, combined libraries were enriched with an NGS enrichment panel kit (RPIP, Illumina), sequenced and quantitative organism detections were analyzed. NGS identified the same bacterial pathogen as traditional testing in all samples, regardless of antibiotic pre-treatment or time collected. Conventional culture methods only identified the pathogen reliably in invasively obtained pleural fluid or endotracheal aspirates. Future application of NGS may allow for non-invasive pathogen detection at a broader range of time points and more targeted antibiotic coverage.
ISSN:0732-8893
1879-0070
1879-0070
DOI:10.1016/j.diagmicrobio.2024.116468