key: cord-0685079-4fyhfxjn
authors: Theresa, L.; Whiteside
title: Procoagulant activity of extracellular vesicles in plasma of patients with SARS-CoV-2 infection
date: 2021-06-03
journal: EBioMedicine
DOI: 10.1016/j.ebiom.2021.103411
sha: 5958d7563fa26fa4e8e9897bf658c96460f606d4
doc_id: 685079
cord_uid: 4fyhfxjn

nan

Extracellular vesicles (EVs) have been of special interest in recent years. Emerging evidence suggests that EVs play a key role in health and disease [1] . Released by all cell types, EVs circulate freely, are present in all body fluids and mediate intercellular communication locally and systemically. Further, EVs reprogram functions of circulating and tissue-bound recipient cells in physiological and pathological conditions [2] . EVs represent a heterogenous population of differently sized nanovesicles with distinct biogenesis that carry diverse molecular and genetic cargo and deliver it to recipient cells [1, 2] . Numbers of circulating EVs increase in inflammatory or infectious diseases, and their molecular/genetic content changes with disease progression. Therefore, EVs are being intensively evaluated as noninvasive liquid biomarkers of disease onset, progression and/or outcome [3] .

EVs are prominently involved in SARS-Cov-2 infection [4] . A proteomic analysis of EVs isolated from plasma of COVID-19 patients identified several molecules involved in the immune response, inflammation, and activation of the coagulation and complement pathways, which are the main mechanisms of COVID-19-associated tissue damage and multiple organ dysfunctions [5] . SARS-CoV-2, unlike other related viruses, shows tropism for alveolar epithelial cells and endothelial cells, which express the human counter-receptor, angiotensin converting enzyme 2 (ACE2). The virus replicates within infected cells causing a severe respiratory syndrome accompanied by systemic inflammation, which may result in multi-organ damage and death [6] . The vascular and endothelial cell dysfunction associated with increased mortality appears to involve the coagulation pathway. Although procoagulant activity of circulating EVs has been known since 1967 [7] , the role these EV play in the COVID-19induced pathology has not been defined.

A report by Balbi and colleagues [8] shows that tissue factor (TF, CD142), a key initiator of the coagulation pathway, is present on the surface of circulating EVs in patients with SARS-CoV-2 infection.

While surface TF expression in circulating EVs accumulating in high procoagulant pathological states was previously described [9] , the Balbi et al. study, identifies TF as a prominent component of the antigenic signature characteristic for circulating EVs in COVID-19 patients and a potentially significant contributor to thrombotic episodes commonly seen in SARS-CoV-2 infections. EVs in sera of 33 COVID(-) and 34 COVID(+) patients were immunocaptured using a cocktail of 37 colored beads, each coated with an antibody specific for one of the 37 target antigens. Fluorescein-labeled antibodies specific for CD9/ CD63/CD81 (i.e., tetraspanins) were used for detection of the EVassociated antigens by flow cytometry. A panel of 7/37 EV-associated antigens (CD142, CD133/1, CD209, CD86, CD69, CD49e and CD20) with the highest scores in EVs of COVID(+) patients was identified. This antigen profile discriminated COVID(+) from COVID(-) patients. Among the 7 antigens in the profile, TF (CD142) had the highest discriminating score. Importantly, expression levels of CD142 on the EV surface correlated with increased serum levels of TNF-alpha in COVID (+) patients. Further, EV-associated TF was biologically active in an assay measuring amidolytic activity of the TF/FVIIa complex, and antibodies neutralizing TF activity significantly reduced procoagulant activity of these EVs. The identification of the EV associated protein signature that reliably discriminates COVID(+) from COVID(-) patients is a significant achievement: TF in EVs emerges as a potential noninvasive biomarker of COVID-19 infection. Even more significant is the finding that TF in EVs from sera of COVID(+) patients was bioactive in ex vivo assays.

Another observation, linking the TF scores and activity of EVs in COVID(+) patients with serum levels of an inflammatory cytokine, TNF alpha, adds special significance to this study. It is known that TF expressed on cell surfaces is "cryptic" and has a low procoagulant activity. To acquire the full-fledged procoagulant activity, membrane-associated TF is "decripted" by an oxidoreductase, protein disulfide isomerase (PDI) [10] . In COVID (+) patients with elevated serum levels of IL-6, IL-8 and TNF-alpha, a "cytokine storm" results in vascular injury and endothelial cell (EC) damage. Activated platelets adhering to damaged ECs release PDI, which enhances the TF DOI Neither do the authors convincingly show that ECs rather than e.g., platelets, which are known to carry TF, are the source of TF(+) EVs. To do so, selective immune capture of EVs derived from ECs or from platelets would be necessary. The multiplex flow cytometry analysis of EVs from COVID(+) patients indicated that immune as well as nonimmune cell types contributed to the total immunocaptured EV population. This emphasizes tremendous heterogeneity of the examined EVs. Based on expression of cell type-associated antigens, the majority of captured EVs originated from ECs or platelets. However, it remains unclear how many EV originating from ECs were TF(+)EVs. Nevertheless, multiplex flow cytometry on beads discriminated COVID(+) from COVID(-) patients by the EV protein profile that was significantly enriched in biologically-active TF only in COVID+ patients. Further, circulating EVs in COVID(+) patients with poor outcome carried significantly higher levels of CD142. The results suggest that TF(+)EVs not only have a diagnostic potential, but might also qualify as a non-invasive prognostic biomarker in SARS-CoV-2 infections. Future studies are necessary to confirm these promising results. Also, Balbi et al. provide a rationale for a future strategy of therapeutically targeting EVs in body fluids of COVID-19 patients. A depletion of pro-thrombotic TF(+)EVs and a pharmacologic blockade of TF activity in these EVs represent a potentially promising future therapeutic strategies.

The author has no conflicts of interest to disclose.

Extracellular microvesicles/exosomes: discovery, disbelief, acceptance, and the future?

The biology, function, and biomedical applications of exosomes

Proteomic analysis of plasma-derived exosomes in defining their role as biomarkers of disease progression, response to therapy and outcome

On the potential role of exosomes in the COVID-19 reinfection/reactivation opportunity

Circulating exosomes are strongly involved in SARS-CoV-2 infection

Endothelial cell contributions to COVID-19

The nature and significance of platelet products in human plasma

Circulating extracellular vesicles are endowed with enhanced procoagulant activity in SARS-CoV-2 infection. EBio-Medicine

Tumorderived tissue factor-bearing microparticles are associated with venous thromboembolic events in malignancy

Protein disulfide isomerase acts as an injury response signal that enhances fibrin generation via tissue factor activation

Partial support was provided by the NIH grant 1U01-DE029759 to TLW.