Litcius/Paper detail

Metabolite profiles associated with disease progression in influenza infection

Chris H. Wendt, Sandra Castro‐Pearson, Jennifer Proper, Sarah Pett, Timothy J. Griffin, Virginia L. Kan, Javier Carbone, Νikolaos Koulouris, Cavan Reilly, James D. Neaton, for the INSIGHT FLU003 Plus Study Group

2021PLoS ONE21 citationsDOIOpen Access PDF

Abstract

BACKGROUND: We performed metabolomic profiling to identify metabolites that correlate with disease progression and death. METHODS: We performed a study of adults hospitalized with Influenza A(H1N1)pdm09. Cases (n = 32) were defined by a composite outcome of death or transfer to the intensive care unit during the 60-day follow-up period. Controls (n = 64) were survivors who did not require transfer to the ICU. Four hundred and eight metabolites from eight families were measured on plasma sample at enrollment using a mass spectrometry based Biocrates platform. Conditional logistic regression was used to summarize the association of the individual metabolites and families with the composite outcome and its major two components. RESULTS: The ten metabolites with the strongest association with disease progression belonged to five different metabolite families with sphingolipids being the most common. The acylcarnitines, glycerides, sphingolipids and biogenic metabolite families had the largest odds ratios based on the composite endpoint. The tryptophan odds ratio for the composite is largely associated with death (OR 17.33: 95% CI, 1.60-187.76). CONCLUSIONS: Individuals that develop disease progression when infected with Influenza H1N1 have a metabolite signature that differs from survivors. Low levels of tryptophan had a strong association with death. REGISTRY: ClinicalTrials.gov Identifier: NCT01056185.

Topics & Concepts

MetaboliteMetabolomeOdds ratioMetabolomicsInternal medicineMedicineBiologyBioinformaticsMetabolomics and Mass Spectrometry StudiesPharmacological Receptor Mechanisms and EffectsInfectious Encephalopathies and Encephalitis