Whole blood transcriptional responses of very preterm infants during late-onset sepsis

F.J. Esteban; S. Ng; T. Strunk; A.H. Lee; E.E. Gill; R. Falsafi; T. Woodman; J. Hibbert; R.E.W. Hancock; A. Currie

doi:10.1371/journal.pone.0233841

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Whole blood transcriptional responses of very preterm infants during late-onset sepsis

Journal article

Open access

Peer reviewed

Whole blood transcriptional responses of very preterm infants during late-onset sepsis

F.J. Esteban, S. Ng, T. Strunk, A.H. Lee, E.E. Gill, R. Falsafi, T. Woodman, J. Hibbert, R.E.W. Hancock and A. Currie

PLoS ONE, Vol.15(6), e0233841

2020

DOI: https://doi.org/10.1371/journal.pone.0233841

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Abstract

Background Host immune responses during late-onset sepsis (LOS) in very preterm infants are poorly characterised due to a complex and dynamic pathophysiology and challenges in working with small available blood volumes. We present here an unbiased transcriptomic analysis of whole peripheral blood from very preterm infants at the time of LOS. Methods RNA-Seq was performed on peripheral blood samples (6–29 days postnatal age) taken at the time of suspected LOS from very preterm infants <30 weeks gestational age. Infants were classified based on blood culture positivity and elevated C-reactive protein concentrations as having confirmed LOS (n = 5), possible LOS (n = 4) or no LOS (n = 9). Bioinformatics and statistical analyses performed included pathway over-representation and protein-protein interaction network analyses. Plasma cytokine immunoassays were performed to validate differentially expressed cytokine pathways. Results The blood leukocyte transcriptional responses of infants with confirmed LOS differed significantly from infants without LOS (1,317 differentially expressed genes). However, infants with possible LOS could not be distinguished from infants with no LOS or confirmed LOS. Transcriptional alterations associated with LOS included genes involved in pathogen recognition (mainly TLR pathways), cytokine signalling (both pro-inflammatory and inhibitory responses), immune and haematological regulation (including cell death pathways), and metabolism (altered cholesterol biosynthesis). At the transcriptional-level cytokine responses during LOS were characterised by over-representation of IFN-α/β, IFN-γ, IL-1 and IL-6 signalling pathways and up-regulation of genes for inflammatory responses. Infants with confirmed LOS had significantly higher levels of IL-1α and IL-6 in their plasma. Conclusions Blood responses in very preterm infants with LOS are characterised by altered host immune responses that appear to reflect unbalanced immuno-metabolic homeostasis.

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Title: Whole blood transcriptional responses of very preterm infants during late-onset sepsis
Authors/Creators: F.J. Esteban (Author/Creator)
S. Ng (Author/Creator)
T. Strunk (Author/Creator)
A.H. Lee (Author/Creator)
E.E. Gill (Author/Creator)
R. Falsafi (Author/Creator)
T. Woodman (Author/Creator)
J. Hibbert (Author/Creator)
R.E.W. Hancock (Author/Creator)
A. Currie (Author/Creator)
Publication Details: PLoS ONE, Vol.15(6), e0233841
Publisher: Public Library of Science
Identifiers: 991005540320907891
Murdoch Affiliation: School of Medical, Molecular and Forensic Sciences
Language: English
Resource Type: Journal article

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Collaboration types: Industry collaboration; Domestic collaboration; International collaboration
Citation topics: 1 Clinical & Life Sciences; 1.23 Antibiotics & Antimicrobials; 1.23.1757 Group B Streptococcus
Web Of Science research areas: Immunology
ESI research areas: Clinical Medicine