Pathogen-specific host response in critically ill patients with blood stream infections: a nested case-control study

Joe M Butler; Hessel Peters-Sengers; Tom D Y Reijnders; Tjitske S R van Engelen; Fabrice Uhel; Lonneke A van Vught; Marcus J Schultz; Pierre-François Laterre; Bruno François; Miguel Sánchez-García; Eleuterio Lombardo; Timothy E Sweeney; Marc J Bonten; W Joost Wiersinga; Dayle Sampson; Leo C Bolero; Thomas Yager; Olaf L Cremer; Brendon P Scicluna; Tom van der Poll

doi:10.1016/j.ebiom.2025.105799

Pathogen-specific host response in critically ill patients with blood stream infections: a nested case-control study

Joe M Butler^*, Hessel Peters-Sengers, Tom D Y Reijnders, Tjitske S R van Engelen, Fabrice Uhel, Lonneke A van Vught, Marcus J Schultz, Pierre-François Laterre, Bruno François, Miguel Sánchez-García, Eleuterio Lombardo, Timothy E Sweeney, Marc J Bonten, W Joost Wiersinga, Dayle Sampson, Leo C Bolero, Thomas Yager, Olaf L Cremer, Brendon P Scicluna, Tom van der Poll

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

BACKGROUND: Knowledge of the contribution of the pathogen to the heterogeneity of the host response to infection is limited. We aimed to compare the host response in critically ill patients with a bloodstream infection (BSI).

METHODS: RNA profiles were determined in blood obtained between one day before and after a positive blood culture. Differential expression and pathway analyses were performed on independent patients' samples by RNA sequencing (discovery) or microarray (validation). Additional patients were included for the discovery and validation of transcriptome classifiers of pathogen-specific BSIs. Twenty biomarkers reflecting key host response pathways were measured in blood.

FINDINGS: We included 341 patients, among which 255 with BSI, 25 with viral infection and 61 non-infectious controls. The cultured pathogen explained 41·8% of the blood transcriptomic variance in patients with BSI. Gene set enrichment analysis showed a global resemblance between monomicrobial BSIs caused by Streptococcus, Staphylococcus aureus and Escherichia coli, which were clearly different from BSI caused by coagulase-negative staphylococci or Enterococcus. BSI by Streptococcus was associated with the highest number of differentially expressed genes, indicating strong innate and adaptive immune activation. An eight-gene streptococcal classifier performed well across different Streptococcus species, and was validated in external cohorts. Plasma biomarker profiling showed that E. coli BSI was associated with the strongest response in the cytokine and systemic inflammation domain, and S. aureus BSI with the strongest endothelial cell activation.

INTERPRETATION: The causative pathogen explains a substantial part of the heterogeneity of the host response in critically ill patients with BSI.

FUNDING: Center for Translational Molecular Medicine and the European Commission.

Original language	English
Article number	105799
Journal	EBioMedicine
Volume	117
Early online date	11 Jun 2025
DOIs	https://doi.org/10.1016/j.ebiom.2025.105799
Publication status	Published - Jul 2025

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Pathogen-specific host response in critically ill patients with blood stream infections: a nested case–control studyFinal published version, 15 MBLicence: CC BY

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Butler, J. M., Peters-Sengers, H., Reijnders, T. D. Y., van Engelen, T. S. R., Uhel, F., van Vught, L. A., Schultz, M. J., Laterre, P.-F., François, B., Sánchez-García, M., Lombardo, E., Sweeney, T. E., Bonten, M. J., Wiersinga, W. J., Sampson, D., Bolero, L. C., Yager, T., Cremer, O. L., Scicluna, B. P., & van der Poll, T. (2025). Pathogen-specific host response in critically ill patients with blood stream infections: a nested case-control study. EBioMedicine, 117, Article 105799. https://doi.org/10.1016/j.ebiom.2025.105799

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abstract = "BACKGROUND: Knowledge of the contribution of the pathogen to the heterogeneity of the host response to infection is limited. We aimed to compare the host response in critically ill patients with a bloodstream infection (BSI).METHODS: RNA profiles were determined in blood obtained between one day before and after a positive blood culture. Differential expression and pathway analyses were performed on independent patients' samples by RNA sequencing (discovery) or microarray (validation). Additional patients were included for the discovery and validation of transcriptome classifiers of pathogen-specific BSIs. Twenty biomarkers reflecting key host response pathways were measured in blood.FINDINGS: We included 341 patients, among which 255 with BSI, 25 with viral infection and 61 non-infectious controls. The cultured pathogen explained 41·8% of the blood transcriptomic variance in patients with BSI. Gene set enrichment analysis showed a global resemblance between monomicrobial BSIs caused by Streptococcus, Staphylococcus aureus and Escherichia coli, which were clearly different from BSI caused by coagulase-negative staphylococci or Enterococcus. BSI by Streptococcus was associated with the highest number of differentially expressed genes, indicating strong innate and adaptive immune activation. An eight-gene streptococcal classifier performed well across different Streptococcus species, and was validated in external cohorts. Plasma biomarker profiling showed that E. coli BSI was associated with the strongest response in the cytokine and systemic inflammation domain, and S. aureus BSI with the strongest endothelial cell activation.INTERPRETATION: The causative pathogen explains a substantial part of the heterogeneity of the host response in critically ill patients with BSI.FUNDING: Center for Translational Molecular Medicine and the European Commission.",

author = "Butler, {Joe M} and Hessel Peters-Sengers and Reijnders, {Tom D Y} and {van Engelen}, {Tjitske S R} and Fabrice Uhel and {van Vught}, {Lonneke A} and Schultz, {Marcus J} and Pierre-Fran{\c c}ois Laterre and Bruno Fran{\c c}ois and Miguel S{\'a}nchez-Garc{\'i}a and Eleuterio Lombardo and Sweeney, {Timothy E} and Bonten, {Marc J} and Wiersinga, {W Joost} and Dayle Sampson and Bolero, {Leo C} and Thomas Yager and Cremer, {Olaf L} and Scicluna, {Brendon P} and {van der Poll}, Tom",

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Butler, JM, Peters-Sengers, H, Reijnders, TDY, van Engelen, TSR, Uhel, F, van Vught, LA, Schultz, MJ, Laterre, P-F, François, B, Sánchez-García, M, Lombardo, E, Sweeney, TE, Bonten, MJ, Wiersinga, WJ, Sampson, D, Bolero, LC, Yager, T, Cremer, OL, Scicluna, BP & van der Poll, T 2025, 'Pathogen-specific host response in critically ill patients with blood stream infections: a nested case-control study', EBioMedicine, vol. 117, 105799. https://doi.org/10.1016/j.ebiom.2025.105799

TY - JOUR

T1 - Pathogen-specific host response in critically ill patients with blood stream infections

T2 - a nested case-control study

AU - Butler, Joe M

AU - Peters-Sengers, Hessel

AU - Reijnders, Tom D Y

AU - van Engelen, Tjitske S R

AU - Uhel, Fabrice

AU - van Vught, Lonneke A

AU - Schultz, Marcus J

AU - Laterre, Pierre-François

AU - François, Bruno

AU - Sánchez-García, Miguel

AU - Lombardo, Eleuterio

AU - Sweeney, Timothy E

AU - Bonten, Marc J

AU - Wiersinga, W Joost

AU - Sampson, Dayle

AU - Bolero, Leo C

AU - Yager, Thomas

AU - Cremer, Olaf L

AU - Scicluna, Brendon P

AU - van der Poll, Tom

PY - 2025/7

Y1 - 2025/7

N2 - BACKGROUND: Knowledge of the contribution of the pathogen to the heterogeneity of the host response to infection is limited. We aimed to compare the host response in critically ill patients with a bloodstream infection (BSI).METHODS: RNA profiles were determined in blood obtained between one day before and after a positive blood culture. Differential expression and pathway analyses were performed on independent patients' samples by RNA sequencing (discovery) or microarray (validation). Additional patients were included for the discovery and validation of transcriptome classifiers of pathogen-specific BSIs. Twenty biomarkers reflecting key host response pathways were measured in blood.FINDINGS: We included 341 patients, among which 255 with BSI, 25 with viral infection and 61 non-infectious controls. The cultured pathogen explained 41·8% of the blood transcriptomic variance in patients with BSI. Gene set enrichment analysis showed a global resemblance between monomicrobial BSIs caused by Streptococcus, Staphylococcus aureus and Escherichia coli, which were clearly different from BSI caused by coagulase-negative staphylococci or Enterococcus. BSI by Streptococcus was associated with the highest number of differentially expressed genes, indicating strong innate and adaptive immune activation. An eight-gene streptococcal classifier performed well across different Streptococcus species, and was validated in external cohorts. Plasma biomarker profiling showed that E. coli BSI was associated with the strongest response in the cytokine and systemic inflammation domain, and S. aureus BSI with the strongest endothelial cell activation.INTERPRETATION: The causative pathogen explains a substantial part of the heterogeneity of the host response in critically ill patients with BSI.FUNDING: Center for Translational Molecular Medicine and the European Commission.

AB - BACKGROUND: Knowledge of the contribution of the pathogen to the heterogeneity of the host response to infection is limited. We aimed to compare the host response in critically ill patients with a bloodstream infection (BSI).METHODS: RNA profiles were determined in blood obtained between one day before and after a positive blood culture. Differential expression and pathway analyses were performed on independent patients' samples by RNA sequencing (discovery) or microarray (validation). Additional patients were included for the discovery and validation of transcriptome classifiers of pathogen-specific BSIs. Twenty biomarkers reflecting key host response pathways were measured in blood.FINDINGS: We included 341 patients, among which 255 with BSI, 25 with viral infection and 61 non-infectious controls. The cultured pathogen explained 41·8% of the blood transcriptomic variance in patients with BSI. Gene set enrichment analysis showed a global resemblance between monomicrobial BSIs caused by Streptococcus, Staphylococcus aureus and Escherichia coli, which were clearly different from BSI caused by coagulase-negative staphylococci or Enterococcus. BSI by Streptococcus was associated with the highest number of differentially expressed genes, indicating strong innate and adaptive immune activation. An eight-gene streptococcal classifier performed well across different Streptococcus species, and was validated in external cohorts. Plasma biomarker profiling showed that E. coli BSI was associated with the strongest response in the cytokine and systemic inflammation domain, and S. aureus BSI with the strongest endothelial cell activation.INTERPRETATION: The causative pathogen explains a substantial part of the heterogeneity of the host response in critically ill patients with BSI.FUNDING: Center for Translational Molecular Medicine and the European Commission.

U2 - 10.1016/j.ebiom.2025.105799

DO - 10.1016/j.ebiom.2025.105799

M3 - Article

C2 - 40505417

SN - 2352-3964

VL - 117

JO - EBioMedicine

JF - EBioMedicine

M1 - 105799

ER -

Pathogen-specific host response in critically ill patients with blood stream infections: a nested case-control study

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