key: cord-293922-knzv4jvj
authors: Zuo, Y.; Warnock, M.; Harbaugh, A.; Yalavarthi, S.; Gockman, K.; Zuo, M.; Madison, J. A.; Knight, J. S.; Kanthi, Y.; Lawrence, D. A.
title: Plasma tissue plasminogen activator and plasminogen activator inhibitor-1 in hospitalized COVID-19 patients
date: 2020-09-02
journal: medRxiv : the preprint server for health sciences
DOI: 10.1101/2020.08.29.20184358
sha: 
doc_id: 293922
cord_uid: knzv4jvj

Background: Patients with coronavirus disease 19 (COVID-19) are at high risk for thrombotic arterial and venous occlusions, while lung histopathology often reveals fibrin-based occlusion of small vessels in patients who succumb to the disease. At the same time, bleeding complications have been observed in some patients. Better understanding the balance between coagulation and fibrinolysis will help inform optimal approaches to thrombosis prophylaxis and potential utility of fibrinolytic-targeted therapies. Objective: To evaluate fibrinolysis among a large cohort of hospitalized COVID-19 patients. Patients and methods: 118 hospitalized COVID-19 patients and 30 healthy controls were included in the study. We measured plasma antigen levels of tissue-type plasminogen activator (tPA) and plasminogen activator inhibitor-1 (PAI-1) and performed spontaneous clot lysis assays. Results: We found markedly elevated levels of tPA and PAI-1 among patients hospitalized with COVID-19. Both factors demonstrated a strong correlation with neutrophil counts and markers of neutrophil activation, but not with D-dimer. High levels of tPA and PAI-1 were associated with worse respiratory status. High levels of tPA, in particular, were also strongly correlated with mortality and with a significant enhancement in spontaneous ex vivo clot lysis. Conclusion: While both tPA and PAI-1 are elevated among COVID-19 patients, extremely high levels of tPA enhance spontaneous fibrinolysis and are significantly associated with mortality in some patients. These data indicate that fibrinolytic homeostasis in COVID-19 is complex with a subset of patients expressing a balance of factors that may favor fibrinolysis and suggests that further study of tPA as a potential biomarker is warranted.

The close relationship between COVID-19 and thrombosis is of significant clinical importance.

There are increasing reports of venous thromboembolism in COVID-19 patients [1, 2] , and arterial thrombosis including strokes and myocardial infarctions have been described [2, 3] .

Histopathology of lung specimens from patients with severe disease demonstrate fibrin-based occlusion of small vessels [4] [5] [6] .

COVID-19 is characterized in most patients by normal levels of coagulation factors, fibrinogen, and platelets suggesting that it is distinct from traditional descriptions of sepsis-induced coagulopathy [7, 8] . There are several (possibly synergistic) mechanisms by which SARS-CoV-2 infection may result in macrovascular and microvascular occlusions including cytokinemediated activation of leukocytes, endothelium, and platelets; hypoxic vasoconstriction; direct activation of endothelial cells by viral transduction [9] ; and potentiation of thrombosis by neutrophil extracellular traps (NETs) [10] [11] [12] [13] . At the same time, bleeding has been described in some patients with COVID-19. For example, a recent multicenter observation of 400 patients hospitalized with COVID-19 demonstrated an overall bleeding rate of 4.8% and a severe bleeding event (WHO grade 3 and 4) rate of 2.3% [14] .

Fibrinolysis is a tightly controlled process whereby a fibrin-rich thrombus is degraded and remodeled by the protease plasmin [15] . This process is regulated by plasminogen activators and inhibitors with the conversion of plasminogen to plasmin being the end result that supports fibrinolysis [15] . The interplay of plasminogen activators-both tissue-type (tPA) and urinarytype (uPA)-and their principal inhibitor, plasminogen activator inhibitor-1 (PAI-1), plays a key role in regulating fibrinolytic activity [15] . Impaired fibrinolysis has been suggested among COVID-19 patients, which could further heighten thrombotic risk. This has been evidenced by markedly reduced clot lysis at 30 minutes via thromboelastography (TEG) in critically-ill patients with COVID-19 [16] . The cause of this fibrinolytic shutdown has yet to be elucidated. Here, we aimed to evaluate the potential roles of tPA and PAI-1 in regulating fibrinolytic homeostasis among COVID-19 patients.

Human samples. Plasma from 118 patients hospitalized with COVID-19 were used in this study. Blood was collected into EDTA by a trained phlebotomist. After completion of hematological testing ordered by the clinician, the remaining plasma was stored at 4°C for up to All rights reserved. No reuse allowed without permission.

(which was not certified by peer review) is the author/funder, who has granted medRxiv a license to display the preprint in perpetuity.

The copyright holder for this preprint this version posted September 2, 2020. . https://doi.org/10.1101/2020.08.29.20184358 doi: medRxiv preprint 48 hours before it was released to the research laboratory. Samples were immediately divided into aliquots and stored at -80°C until testing. All 118 patients had a confirmed COVID-19 diagnosis based on FDA-approved RNA testing. This study complied with all relevant ethical regulations and was approved by the University of Michigan IRB (HUM00179409). Healthy volunteers were recruited through a posted flyer; exclusion criteria for controls included history of a systemic autoimmune disease, active infection, and pregnancy. The 30 controls included 20 females and 10 males, mean age of 41.7 ± 14.4. All plasma samples were treated with solvent/detergent (0.3% v/v tri-(n-butyl) phosphate and 1% Triton X-100) to inactivate the virus [17] . was added to the plate, followed by incubating with phycoerythrin-conjugated streptavidin. The plate was read with a Luminex® 100 System; the setting was 100 μL sample size and 100 events per well.

To determine the rate of spontaneous lysis, 40 µL of diluted plasma (1:1 in TBS) was added to a microtiter plate and pre-read at 405 nm. Then, 40 µL of 25 nM alpha human thrombin (Haemtech) and 15 mM CaCl2 was added and incubated at 37°C for 30 minutes, and the absorbance was read at 405 nm. Twenty µL of TBS was added and the plate was read again after 30 minutes and then at 60-minute intervals up to 8 hours.

Human S100A8/S100A9 Heterodimer DuoSet ELISA (DY8226-05, R&D Systems) according to the manufacturer's instructions.

When two groups were present, normally-distributed data were analyzed by two-sided t test and skewed data were analyzed by Mann-Whitney test or Wilcoxon test. For three or more groups, analysis was by one-way ANOVA or Kruskal-Wallis test with correction for multiple comparisons. Correlations were tested by Spearman's method. Data analysis was with GraphPad Prism software version 8. Statistical significance was defined as p<0.05. All rights reserved. No reuse allowed without permission.

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The copyright holder for this preprint this version posted September 2, 2020. . https://doi.org/10.1101/2020.08.29.20184358 doi: medRxiv preprint

Utilizing established Luminex platforms, we measured total PAI-1 and tPA levels in the plasma of 118 patients hospitalized with COVID-19 and 30 healthy controls. Of the 118 COVID-19 patients, the mean age was 60.7 with a standard deviation of 17.1 (range 25-95); 54 were female (45.8%). In terms of respiratory status, 45.2% were supported by mechanical ventilation, 7.6% were receiving high-flow oxygen, 27.1% were using standard nasal cannula, and 23.7%

were breathing room air at the time of sample collection. Markedly elevated levels of both PAI-1 and tPA were detected in patients with COVID-19 as compared with healthy controls ( Figure   1A -B), which included a significant correlation between levels of PAI-1 and tPA among COVID-19 patients ( Figure 1C ). In summary, PAI-1 and tPA are markedly elevated in patients hospitalized with COVID-19.

We assessed potential correlations with D-dimer and platelet count. To draw integral comparisons, we limited the analysis of clinical laboratory measurements to those performed on the same day as plasma used for the PAI-1 and tPA assays. No significant correlation was found between Ddimer and either PAI-1 or tPA (Figure 2A-B) . We did observe a strong correlation between PAI-1 (but not tPA) and platelet count (Figure 2C-D) . Given that activated neutrophils and their products can exert anti-fibrinolytic effects [18] , we next asked how absolute neutrophil count and calprotectin (a marker of neutrophil activation) compared to tPA and PAI-1. We detected a strong positive correlation between both PAI-1 and tPA and same-day absolute neutrophil count Levels of PAI-1 and tPA associate with severe disease and worse outcomes. Compared with patients breathing room air, patients requiring oxygen had significantly higher levels of PAI-1 ( Figure 3B ), but not tPA ( Figure 3C ) nor D-dimer ( Figure 3A) . Beyond mode of respiratory support, oxygenation efficiency can also be measured by comparing pulse oximetry (SpO2) to the fraction of inspired oxygen (FiO2). We tested the correlation between D-dimer, PAI-1 and SpO2/FiO2 ratio and found a strong negative association (Figure 3D-E) . A negative association was also appreciated between oxygenation efficiency and tPA, albeit less robust than for PAI-1 and D-dimer ( Figure 3F) . Among the 118 patients, 24 died, 92 were discharged, and two All rights reserved. No reuse allowed without permission.

(which was not certified by peer review) is the author/funder, who has granted medRxiv a license to display the preprint in perpetuity.

The copyright holder for this preprint this version posted September 2, 2020. . https://doi.org/10.1101/2020.08.29.20184358 doi: medRxiv preprint remained hospitalized at the time of this writing. Significantly higher levels of both PAI-1 and tPA were observed among patients who expired as compared with those who were discharged, with this difference being especially robust for tPA (Figure 3H-I) . Surprisingly, we did not see a significant difference in D-dimer level between those two groups ( Figure 3G) . In summary, high levels of tPA and PAI-1 were associated with worsening respiratory status and poor clinical outcomes.

High tPA COVID-19 samples have enhanced spontaneous fibrinolysis. Finally, we asked whether COVID-19 plasma with the highest tPA levels might demonstrate enhanced spontaneous fibrinolysis as compared with low-tPA COVID-19 plasma or control plasma. A spontaneous fibrinolysis assay was performed on 10 COVID-19 plasma samples with high tPA, 10 COVID-19 samples with low tPA, and 10 healthy control plasma samples. Interestingly, the high-tPA COVID-19 samples significantly enhanced spontaneous fibrinolysis as compared with low-tPA and healthy control plasma samples (Figure 4A-B) .

Normal lung physiology has a pro-fibrinolytic tendency [19] . However, during acute respiratory distress syndrome (ARDS) impaired fibrinolysis results in accumulation of fibrin that promotes hyaline membrane formation and alveolar injury [20] . Fibrin is removed by plasmin. It is believed that depressed fibrinolysis in ARDS is at least partially driven by increased circulating PAI-1 that exerts a negative effect on the plasminogen activation system [19] . Indeed, elevated PAI-1 is an independent risk factor for poor ARDS outcomes [21] . Elevated PAI-1 and its associated hypofibrinolytic state were observed in the 2002 SARS-CoV epidemic [22] , while recent characterizations of COVID-19 patients have suggested impaired global fibrinolysis [16, 23] .

Interestingly, in our large cohort of hospitalized COVID-19 patients, we observed elevated levels of not only PAI-1, but also tPA. While high PAI-1 and D-dimer tracked most closely with impaired oxygenation efficiency, tPA was the best predictor of death. A recent study of hospitalized COVID-19 patients also detected elevations of both PAI-1 and tPA, particularly among critically-ill COVID-19 patients [23] ; however, the mechanistic role of the elevated tPA among COVID-19 patients was not specifically investigated [23] . The level of tPA we detected is striking and much higher than described in prior reports. Notably levels are even higher than is observed in trauma patients who have exaggerated fibrinolytic activity and in patients with hantavirus cardiopulmonary syndrome, which carries high alveolar hemorrhage risk [24] [25] [26] .

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The major source of these high levels of tPA among COVID-19 patients is likely endothelial cells. The source of PAI-1 could also be the endothelium or perhaps release from activated platelets (as we found a strong correlation between PAI-1 and platelet counts). High PAI-1 expression in other cell types such as macrophages has been reported during hantavirus infections [24] . One hallmark of COVID-19 ARDS is the sequestration of leukocytes, particularly neutrophils, in the microvasculature of the lung-contributing to alveolar injury and unrestricted inflammation [21] . This local proinflammatory environment is further exaggerated by the formation of NETs and results in massive release of proinflammatory cytokines [6] . Those cytokines trigger endothelial cell activation and likely promote local release of tPA and PAI-1 [6, 27] . Unsurprisingly, we observed a strong correlation between tPA/PAI-1 and both absolute neutrophil counts and circulating calprotectin, a neutrophil activation marker. In addition to endothelial activation, it is possible that direct infection and destruction of endothelial cells by SARS-CoV-2 may also potentiate the release of tPA and PAI-1 [9] .

While the prothrombotic risk associated with COVID-19 is well recognized, the risk of bleeding should not be ignored. One recent large multicenter study observed an overall bleeding risk of 4.8% among hospitalized COVID-19 patients and this risk increased to 7.6% among critically-ill patients [14] . Elevated D-dimer was associated with both thrombotic and bleeding complications [14] . It has been suggested that high PAI-1 levels overcome the effects of local tPA and produce a net prothrombotic hypofibrinolytic state in COVID-19 patients [23] . However, we here found a subset of COVID-19 patients with extremely high levels of tPA in which fibrinolysis seems to dominate. This may at least partially explain the enhanced bleeding risk observed in some groups of patients with COVID-19.

Because the COVID-19 associated prothrombotic risk is known, prophylactic anticoagulation has become part of standard COVID-19 treatment. High rates of thromboembolic events from early studies prompted some experts to recommend a more intensive dose of anticoagulation among COVID-19 patients [2] . We would urge caution regarding this recommendation (pending randomized studies) as the coagulopathy of COVID-19 is complex and potentially dynamic.

Therapies aimed at promoting fibrinolysis, such as administration of aerosolized or intravenous tPA, have been trialed in ARDS models where there have been some promising preclinical results [28, 29] . Profibrinolytic therapy has been suggested as a potential beneficial therapy in COVID-19 patients suffering from ARDS [21] and is currently being tested in multiple clinical trials (https://clinicaltrials.gov/ct2/results?cond=Covid19&term=tpa). We have now found that a All rights reserved. No reuse allowed without permission.

(which was not certified by peer review) is the author/funder, who has granted medRxiv a license to display the preprint in perpetuity.

The copyright holder for this preprint this version posted September 2, 2020. . https://doi.org/10.1101/2020.08.29.20184358 doi: medRxiv preprint hyperfibrinolytic state exists in some COVID-19 patients. Targeted therapies that promote fibrinolysis therefore need to be selective and cautious to minimize bleeding risk. Finally, our data suggests that high systemic tPA may be a biomarker for poor clinical outcomes and supports further studies of tPA levels during the course of disease progression. and DAL conceived the study and analyzed data. All authors participated in writing the manuscript and gave approval before submission.

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(which was not certified by peer review) is the author/funder, who has granted medRxiv a license to display the preprint in perpetuity.

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The copyright holder for this preprint this version posted September 2, 2020. . https://doi.org/10.1101/2020.08.29.20184358 doi: medRxiv preprint (which was not certified by peer review) is the author/funder, who has granted medRxiv a license to display the preprint in perpetuity.

The copyright holder for this preprint this version posted September 2, 2020. . https://doi.org/10.1101/2020.08.29.20184358 doi: medRxiv preprint (which was not certified by peer review) is the author/funder, who has granted medRxiv a license to display the preprint in perpetuity.

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