| Journal of Intensive Care | 卷:10 |
| A prospective observational cohort study to identify inflammatory biomarkers for the diagnosis and prognosis of patients with sepsis | |
| Dirk Valkenborg1 Reinoud Cartuyvels2 Inge Grondman3 Leo A. B. Joosten3 Mihai G. Netea3 Johan Vanwalleghem4 Agnes Meersman5 Peter Messiaen6 Valentino D’Onofrio6 Inge C. Gyssens6 Gökhan Ertaylan7 Murih Pusparum7 Dries Heylen7 | |
| [1] Data Science Institute, Hasselt University; | |
| [2] Department of Clinical Biology, Jessa Hospital; | |
| [3] Department of Internal Medicine and Radboud Center for Infectious Diseases, Radboud University Medical Center; | |
| [4] Department of Nephrology, Jessa Hospital; | |
| [5] Emergency Department, Jessa Hospital; | |
| [6] Faculty of Medicine and Life Sciences, Hasselt University; | |
| [7] Unit Health, Flemish Institute for Technological Research (VITO); | |
| 关键词: Biomarkers; Sepsis; Inflammation; Disease severity; | |
| DOI : 10.1186/s40560-022-00602-x | |
| 来源: DOAJ | |
【 摘 要 】
Abstract Background Sepsis is a life-threatening organ dysfunction. A fast diagnosis is crucial for patient management. Proteins that are synthesized during the inflammatory response can be used as biomarkers, helping in a rapid clinical assessment or an early diagnosis of infection. The aim of this study was to identify biomarkers of inflammation for the diagnosis and prognosis of infection in patients with suspected sepsis. Methods In total 406 episodes were included in a prospective cohort study. Plasma was collected from all patients with suspected sepsis, for whom blood cultures were drawn, in the emergency department (ED), the department of infectious diseases, or the haemodialysis unit on the first day of a new episode. Samples were analysed using a 92-plex proteomic panel based on a proximity extension assay with oligonucleotide-labelled antibody probe pairs (OLink, Uppsala, Sweden). Supervised and unsupervised differential expression analyses and pathway enrichment analyses were performed to search for inflammatory proteins that were different between patients with viral or bacterial sepsis and between patients with worse or less severe outcome. Results Supervised differential expression analysis revealed 21 proteins that were significantly lower in circulation of patients with viral infections compared to patients with bacterial infections. More strongly, higher expression levels were observed for 38 proteins in patients with high SOFA scores (> 4), and for 21 proteins in patients with worse outcome. These proteins are mostly involved in pathways known to be activated early in the inflammatory response. Unsupervised, hierarchical clustering confirmed that inflammatory response was more strongly related to disease severity than to aetiology. Conclusion Several differentially expressed inflammatory proteins were identified that could be used as biomarkers for sepsis. These proteins are mostly related to disease severity. Within the setting of an emergency department, they could be used for outcome prediction, patient monitoring, and directing diagnostics. Trail registration number: clinicaltrial.gov identifier NCT03841162.
【 授权许可】
Unknown
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