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The proteomic landscape of blood monocytes in community-acquired pneumonia

作者
Osoul Chouchane,Erik H.A. Michels,Giuseppe G. F. Leite,Alex F. de Vos,Justin de Brabander,Joe M. Butler,Xanthe Brands,Bastiaan W. Haak,Augustijn M. Klarenbeek,W. Joost Wiersinga,Brendon P. Scicluna,Cornelis van ′t Veer,Kathrine F. Kaas,Valdemaras Petrosius,Erwin M. Schoof,Tom van der Poll
出处
期刊:The European respiratory journal [European Respiratory Society]
卷期号:: 2500335-2500335
标识
DOI:10.1183/13993003.00335-2025
摘要

Introduction Monocytes play a pivotal role in the regulation of inflammation and pathogen clearance during infection. Knowledge of the human monocyte proteome during infection is limited. We present a comprehensive proteome profile of blood monocytes from patients with community-acquired pneumonia (CAP), one of the most common infectious diseases, and controls without infection. Methods Monocytes were purified from blood of patients with CAP within 16 h of admission to a general hospital ward and from controls matched for sex, age and comorbidities. Monocyte proteins were measured by liquid chromatography/mass spectrometry. The transcriptome was analysed in the same samples by RNA sequencing. Monocytes were stimulated with lipopolysaccharide for 24 h, after which cytokines were measured in the supernatant. Results We analysed the monocyte proteome of 34 CAP patients and 23 controls. Of 7315 annotated proteins 1340 (18.3%) were differentially abundant between groups. Functional enrichment analyses revealed a marked downregulation of mitochondrial respiration processes in patients’ monocytes; pathways pertaining to cell cycle, cytokine signalling and cell death were upregulated in patients’ monocytes. Monocyte mRNA levels correlated poorly with the abundance of corresponding proteins and associated functional pathways, raising caution regarding interpretation of functionality estimates based on transcriptome analyses. Differential expression of monocyte proteins had functional and clinical implications as indicated by associations with cytokine production capacity, disease severity and time to clinical stability. Conclusion This study provides a publicly available monocyte protein atlas that can serve as a resource for future research on monocyte functions during infection.

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