Thrombosis pathways in COVID-19 vs. influenza-associated ARDS: A targeted proteomics approach

Emma Rademaker; Dennis J Doorduijn; Nuray Kusadasi; Coen Maas; Julia Drylewicz; Albert Huisman; Imo E Hoefer; Marc J M Bonten; Lennie P G Derde; Suzan H M Rooijakkers; Olaf L Cremer

doi:10.1111/jth.15671

Thrombosis pathways in COVID-19 vs. influenza-associated ARDS: A targeted proteomics approach

J Thromb Haemost. 2022 May;20(5):1206-1212. doi: 10.1111/jth.15671. Epub 2022 Feb 27.

Authors

Affiliations

¹ Julius Center, University Medical Center Utrecht, Utrecht, The Netherlands.
² Department of Medical Microbiology, University Medical Center Utrecht, Utrecht, The Netherlands.
³ Department of Intensive Care, University Medical Center Utrecht, Utrecht, The Netherlands.
⁴ Department of Clinical Chemistry and Haematology, University Medical Center Utrecht, Utrecht, The Netherlands.
⁵ Center for Translational Immunology, University Medical Center Utrecht, Utrecht, The Netherlands.

Abstract

Background: Pulmonary embolism (PE) occurs in one-third of critically-ill COVID-19 patients. Although prior studies identified several pathways contributing to thrombogenicity, it is unknown whether this is COVID-19-specific or also occurs in ARDS patients with another infection.

Objective: To compare pathway activity among patients having COVID-19 with PE (C19PE+), COVID-19 without PE (C19PE-), and influenza-associated ARDS (IAA) using a targeted proteomics approach.

Methods: We exploited an existing biorepository containing daily plasma samples to carefully match C19PE+ cases to C19PE- and IAA controls on mechanical ventilation duration, PEEP, FiO2, and cardiovascular-SOFA (n = 15 per group). Biomarkers representing various thrombosis pathways were measured using proximity extension- and ELISA-assays. Summed z-scores of individual biomarkers were used to represent total pathway activity.

Results: We observed no relevant between-group differences among 22 biomarkers associated with activation of endothelium, platelets, complement, coagulation, fibrinolysis or inflammation, except sIL-1RT2 and sST2, which were lower in C19PE- than IAA (log2-Foldchange -0.67, p = .022 and -1.78, p = .022, respectively). However, total pathway analysis indicated increased activation of endothelium (z-score 0.2 [-0.3-1.03] vs. 0.98 [-2.5--0.3], p = .027), platelets (1.0 [-1.3-3.0] vs. -3.3 [-4.1--0.6], p = .023) and coagulation (0.8 [-0.5-2.0] vs. -1.0 [-1.6-1.0], p = .023) in COVID-19 patients (C19PE+/C19PE- groups combined) compared to IAA.

Conclusion: We observed only minor differences between matched C19PE+, C19PE-, and IAA patients, which suggests individual biomarkers mostly reflect disease severity. However, analysis of total pathway activity suggested upregulation of some distinct processes in COVID-19 could be etiologically related to increased PE-risk.

Keywords: COVID-19; influenza; pulmonary embolism; respiratory distress syndrome; thrombosis.

MeSH terms

Biomarkers
COVID-19* / complications
Humans
Influenza, Human* / complications
Influenza, Human* / diagnosis
Proteomics
Pulmonary Embolism* / diagnosis
Respiratory Distress Syndrome*
SARS-CoV-2
Thrombosis*

Substances

Biomarkers