key: cord-0987349-eisju9xy authors: Stiel, Laure; Rabouel, Yannick; Debliquis, Agathe; Pointurier, Valentin; Mootien, Joy; Kuteifan, Khaldoun title: NEUT-SFL in Patients with COVID-ARDS: A Novel Biomarker for Thrombotic Events? date: 2021-11-17 journal: Dis Markers DOI: 10.1155/2021/4361844 sha: 753f50f04efe0712ec6b0f7aedabcf4d4a246631 doc_id: 987349 cord_uid: eisju9xy The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is an enveloped RNA virus first identified in December 2019 in Wuhan, China, and responsible for coronavirus disease 2019 (COVID-19). The ongoing COVID-19 pandemic is impacting healthcare worldwide. Patients who develop coagulopathy have worse outcomes. The pathophysiology of COVID-19 suggests a strong interplay between hemostasis and immune cells, especially neutrophils. Our purpose was to assess neutrophil fluorescence as a potential biomarker of deep vein thrombosis (DVT) in patients with COVID-acute respiratory distress syndrome (COVID-ARDS). Sixty-one patients with COVID-ARDS admitted to the four intensive care units (ICUs) of a French general hospital were included in this prospective study. Neutrophil activation was assessed by measuring neutrophil fluorescence (NEUT-Side Fluorescence Light, NEUT-SFL) with a specific fluorescent dye staining analyzed by a routine automated flow cytometer Sysmex XN-3000™ (Sysmex, Kobe, Japan). DVT was diagnosed by complete duplex ultrasound (CDU). We found that NEUT-SFL was elevated on admission in patients with COVID-ARDS (49.76 AU, reference value 46.40 AU, p < 0.001), but did not differ between patients with DVT (49.99 AU) and those without (49.52 AU, p = 0.555). NEUT-SFL is elevated in patients with COVID-ARDS, reflecting neutrophil activation, but cannot be used as a marker of thrombosis. Because neutrophils are at interface between immune response and hemostasis through release of neutrophil extracellular traps, monitoring their activation could be an interesting approach to improve our management of coagulopathy during COVID-ARDS. Further research is needed to better understand the pathophysiology of COVID-19 and identify high-performance biomarkers. The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is a member of the beta-coronavirus class, a family of enveloped positive-sense single-stranded RNA viruses (B). SARS-CoV-2 is responsible for the coronavirus disease 2019 . COVID-19 spread from Wuhan, China, where it was first identified in December 2019 and is at the origin of the ongoing COVID-19 pandemic [1, 2] . The clinical spectrum of COVID-19 ranges from asymptomatic disease to severe viral pneumonia with acute respiratory distress syndrome (ARDS) [3] . While COVID-19 typically begins as a respiratory infection, it may progress to multisystemic disease. Immune response is aimed at viral elimination and recovery. Nevertheless, overwhelming inflammatory and immune response can lead to widespread tissue damage, which in turn may be implicated in disease progression and mortality [4, 5] . This inflammatory response is associated with activation of coagulation, and indeed, a high percentage of patients with COVID-ARDS develop life-threatening thrombotic complications associated with poor prognosis [6] [7] [8] . Deep vein thrombosis (DVT) and pulmonary embolism (PE) represent the most serious thrombotic complications [7] . Arterial thrombosis, as well as clotting of catheters, dialysis membranes, or extracorporeal membrane oxygenation circuits, has also been observed [6, 9, 10] . The coagulopathy of SARS-CoV-2 infection is characterized by prominent elevation of D-dimers and fibrinogen, whereas classical coagulation biomarkers, such as prothrombin time or platelet count, remain within normal range [8, 11, 12] . This suggests uncontrolled activation of coagulation resulting in widespread microvascular thrombosis. The mechanisms of this coagulopathy are still unclear, and many molecular patterns seem to be involved, including dysregulation of the renin-angiotensin-aldosterone system (RAAS) caused by fixation of SARS-CoV-2 to angiotensinconverting enzyme 2 receptor (ACE2), oxidative stress leading to endothelial damage, and complement activation [13] [14] [15] . Most of these pathophysiological hypotheses suggest a strong interplay between immune response and hemostasis, termed immunothrombosis [16] . In this model, cytokines, platelets, immune cells, especially polymorphonuclear neutrophils (PMNs), and pathogen-associated molecular patterns induce thrombosis. Immunothrombosis participates in host defense but, if uncontrolled, can become maladaptive and induce organ dysfunction [16, 17] . The role of neutrophils in vascular cell dysfunction and aberrant host response has been studied more specifically during septic shock and septic shock-induced disseminated intravascular coagulopathy (DIC) [16, 18, 19] . Elevation of Neutrophil-Side Fluorescent Light (NEUT-SFL) was identified as a biomarker of neutrophil activation and is associated with septic shock-induced DIC [20] . During severe COVID-19, neutrophilia is predictive of severity. Pathology findings describe neutrophils in the capillaries in the lungs of autopsied COVID-19 patients [21, 22] . These observations suggest that the neutrophil could have a central role in aberrant host response inducing thrombosis in patients with COVID-ARDS. The main objective of this study was to evaluate neutrophil fluorescence as a biomarker of deep vein thrombosis (DVT) in patients admitted for COVID-ARDS to the four intensive care units (ICUs) of the Groupe Hospitalier de la Région de Mulhouse Sud Alsace (GHRMSA). Sixty-one adult patients admitted for COVID-ARDS to the four ICUs of GHRMSA were included in this study. There were no exclusion criteria. COVID-19 diagnosis was confirmed by a positive reverse-transcriptasepolymerisation chain reaction assay of a nasopharyngeal swab for SARS-CoV-2. Patients were managed according to current guidelines. Complete blood count (CBC) and complete duplex ultrasound (CDU) were performed in all patients. The Ethics Committee of our institution approved this study. Characteristics. Demographic characteristics and biological parameters were collected at baseline and in the 24 hours preceding CDU exam. Simplified Acute Physiology Score (SAPS) II and Sequential Organ Failure Assessment (SOFA) score were calculated on admission. 2.3. DVT Definition and CDU. DVT was defined as a lowerlimb vein thrombosis or as a nonleg vein thrombosis diag-nosed by CDU. Only obstructive internal jugular or subclavian vein thrombosis was considered for nonleg vein thrombosis. CDU examination was performed using the General Electric vivid S6® device by two physicians of the vascular medical team of our institution. 2.4. Other Thrombotic Events. We did not systematically search for or record other thrombotic events. Imaging was performed if a thrombotic event was suspected based on clinical or laboratory parameters. Patients with suspected pulmonary embolism (PE) had CT pulmonary angiography (CTPA); patients with suspected arterial ischemia were evaluated by CT angiography. 2.5. Anticoagulation Treatment. All patients received anticoagulant treatment at admission. The choice between low molecular weight heparin (LMWH) and unfractionated heparin (UFH) treatment was determined by creatinine clearance with a 50 mL/min cut-off. Usual direct oral anticoagulants or vitamin K antagonists were substituted by LMWH or UFH. Usual antiplatelet treatment was pursued. Classic prophylactic anticoagulant therapy was defined as the administration of standard dose LMWH or UFH. Reinforced prophylactic anticoagulant therapy was defined as the administration of double dose LMWH or UFH for a targeted heparin activity between 0.2 and 0.3 IU/mL. Curative anticoagulant therapy was defined as the administration of high-dose LMWH with a targeted anti-Xa activity between 0.6 and 1.0 IU/mL or UFH with a targeted heparin activity between 0.3 and 0.5 IU/mL for patients with a history atrial fibrillation or VTE or between 0.4 and 0.6 IU/mL for patients with active VTE or mechanical cardiac valve. 2.6. Neutrophil Fluorescence Analysis. Blood was sampled in ethylene-diamine-tetraacetic acid (7.2 mg/4 mL) tubes on admission and on the day of the CDU. A complete blood count (CBC) was performed on a routine automated Sysmex XN-3000™ analyzer (Sysmex, Kobe, Japan) based on impedance and fluorescence flow cytometry technologies according to the manufacturer's instructions. The analyzer uses flow cytometry technology to determine the white blood cell count. Sysmex XN-3000™ is equipped with a red scatter laser light with a wavelength of 633 nm (front and side). After permeabilization by a specific Sysmex lysis reagent, three signals are recorded in the white cell differential scattergrams: forward-scattered light (FSC) (cell size), SSC (granularity), and Side Fluorescence Light (SFL) (DNA/RNA content). Neutrophil chromatin decondensation is assessed by measuring the NEUT-SFL signal generated by the incorporation of a fluorochrome-based polymethine dye that targets unpacked DNA within the permeabilized cells [23] . Binding of the dye depends on the number of available binding sites on the DNA strand; NEUT-SFL is thus a surrogate of neutrophil activation. According to the manufacturer, NEUT-SFL values in normal neutrophils are very stable [24] . The mean reference value is 46.40 arbitrary units (AU). This value has previously been validated by analyzing NEUT-SFL in more than 1300 consecutive blood samples [20] . Three control samples are CTPA was performed in twenty-one patients. Five of them had PE, of whom two had no DVT. Nine other thrombotic events were observed: seven patients who received haemodialysis presented at least one clotting of the circuit, one patient suffered multiple arterial distal necrosis, and one patient supported by veno-venous extracorporeal membrane oxygenation presented thrombotic occlusion of the centrifugal pump. In total, thirty-five (57.4%) patients developed at least one thrombotic event during their ICU stay. According to the manufacturer, the NEUT-SFL mean reference value in normal neutrophils is 46.40 arbitrary units (AU) (manufacturer data). On admission, NEUT-SFL was significantly increased in patients with COVID-ARDS (49.76 AU, p < 0:001). Nevertheless, NEUT-SFL on admission was not significantly different between patients with DVT and those without (49.52 AU versus 49.99 AU, DVT vs. non-DVT, respectively, p = 0:555) (Figure 1(a) ). There was no significant difference in NEUT-SFL between groups on the day of CDU (51.04 AU versus 52.34 AU, respectively, p = 0:178) (Figure 1(b) ). The area under the ROC curve was 0.5853 (0.41L6-0.7540) (p = 0:3279) for DVT diagnosis at admission and 0.6000 (0.4316-0.7684) (p = 0:2470) on the day of the CDU. There was also no significant difference in NEUT-SFL between patients who presented any thrombotic event (49.67 AU) and those without thrombosis (49.90 AU, p = 0:782) (Figures 1(c) and 1(d) ). Leukocyte and neutrophil counts were not significantly different between patients with versus without DVT at admission or on the day of CDU (Table 1) . Nevertheless, an elevated neutrophil-to-lymphocyte ratio (NLR) at admission was associated with higher mortality (Figure 1(f) , p = 0:0186) but was not associated DVT (Figure 1(e) ). In this prospective study, NEUT-SFL was found to be elevated at admission in patients with COVID-ARDS. The values of NEUT-SFL were similar to those reported during septic shock, reflecting neutrophil activation during COVID-19 [20, 25] . In patients with septic shock, elevated NEUT-SFL was shown to be associated with DIC [20] . In our cohort, NEUT-SFL did not differ between patients with and those without DVT. Based on these observations and on the coagulation parameters previously described [6] [7] [8] , the mechanisms of coagulation activation in COVID-ARDS and in septic shock-induced DIC would appear to be different. Indeed, during COVID-ARDS, fibrinogen, and Ddimers are elevated, while platelet count initially remains normal. Some patients tend to have values at the lower end of the normal range, but the severe thrombocytopenia seen in DIC is rarely observed [26] . These findings suggest that overwhelming activation of coagulation could be a local phenomenon with a "local DIC" phenotype, especially in the lungs [27] . This localized thrombosis could probably be mediated by vascular cells, especially endothelial cells and infiltrating neutrophils [21, 28] . Exploring infiltrating neutrophils, for example, in pulmonary aspirates, may be an interesting approach to improve our understanding of the disease. In this regard, although DVT is a frequent and worrisome thrombotic complication of severe COVID, it may not be representative of immunothrombosis as described in septic shock-induced DIC. Although clinical diagnosis of DVT is routinely available, macrothrombosis may not be the best way to monitor the coagulation state of severe patients with progressing disease. Nevertheless, considering COVID-induced coagulopathy as a local phenomenon remains a matter of debate [27, 29] . The multisystemic clinical features of COVID-19 suggest a systemic vascular disease with diffuse endothelial dysfunction associated with microangiopathy, with predominant lung tropism [30, 31] . Neutrophils could have an important role in this vascular disease. Indeed, neutrophilia is predictive of poor outcome in COVID patients, and elevated NLR is associated with mortality [32, 33] . We confirm this result in our cohort. Our observations and others together suggest that enhanced neutrophil infiltration at the site of infection, associated with extensive lymphocyte depletion, may contribute 3 Disease Markers to aberrant immunothrombosis during COVID-19. Elevation of NEUT-SFL indicates activation of PMNs, which promotes immune-mediated blood coagulation activation via different mechanisms: activated PMNs express tissue factor, leading to endothelial cell damage through degranulation and production of reactive oxygen species [34] . Activated PMNs also release microparticles and neutrophil extracellular traps (NETs) [16, 18, 35] . Furthermore, they interact with platelets, forming activated platelet-neutrophil complexes that trigger an immune response to infection through neutrophil recruitment and NET production [36] . Barnes et al. reported a histological description of lungs from 3 necropsies of patients with COVID-ARDS in April 2020 [21] . They described interstitial neutrophilic infiltration with small vessel occlusions containing PMNs and neutrophil fragments consistent with NETs [21, 37] . It remains uncertain whether these modifications are specific to SARS-CoV-2 infection or a final common stage in the thromboinflammatory response to fatal viral infections [14, 28] . Neutrophil infiltration is probably mediated by downregulation of ACE2 expressed by pulmonary epithelial cells on SARS-CoV-2 infection [38, 39] . Although the detection of NETs remains controversial, and the evidence in COVID-ARDS is limited (albeit growing), PMNs seem to play an important role in the pathophysiology of complications of COVID-19. Underlying comorbidities like diabetes or cardiovascular diseases, associated with a risk of severe forms of COVID-19, also contribute to persistent exaggerated neutrophil activation [38] . Altogether, NEUT-SFL does not seem to be a good marker of DVT during COVID-19. Perhaps it is not specific enough, because it reflects the different pathways of PMN activation (e.g., phagocytosis, NETosis and degranulation, to mention but a few) [19, 40] . Biomarkers of NETs could be more representative of the role of PMNs in COVID hypercoagulability, as previously reported in other forms of ARDS [41] . Recent postmortem findings confirm the presence of NETs in the lungs of patients who died from COVID-19 [42] . Elevation of two indirect markers of NETosis, namely, cell-free DNA and MPO-DNA, in the plasma of patients with severe forms of COVID-19 has also been reported [43] . Nevertheless, because of the ongoing COVID-19 pandemic, it is of paramount importance to identify routinely available biomarkers that could improve physician decision-making for treatment or orientation of patients. Our preliminarily observational study has some limitations and was not designed to demonstrate the pathophysiology of thrombosis during COVID-ARDS. Further studies exploring more haematological markers in a large panel of patients could help to guide clinical decision-making at the bedside, pending a more comprehensive approach to the disease based on translational research. To the best of our knowledge, we report the first cohort to investigate the association between neutrophil activation, as measured by NEUT-SFL, and DVT in patients with COVID-ARDS. Our data highlights NEUT-SFL as a marker of neutrophil activation during COVID-ARDS, but not as a marker of DVT or other macrothrombosis. NEUT-SFL cannot be used as a marker of thrombosis in COVID-19 patients. COVID-ARDS represents a state of overwhelming inflammatory response to infection associated with hypercoagulation, which induces multiorgan failure. For now, lymphocyte count, NLR, and D-dimers offer the better prognostic information in the management of the disease, but they are not sufficient. Therefore, new biomarkers measuring vascular cell activation are needed to monitor the state of the disease and perhaps enable case-by-case management. Neutrophils nonetheless remain an interesting target for further research, because they are at interface between immune response and hemostasis. Further translational research is needed to better understand the pathophysiology of COVID-19. Data are available on request. The authors declare that they have no conflicts of interest. 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