key: cord-0839051-tr58peem
authors: Dogra, Siddhant; Jain, Rajan; Cao, Meng; Bilaloglu, Seda; Zagzag, David; Hochman, Sarah; Lewis, Ariane; Melmed, Kara; Hochman, Katherine; Horwitz, Leora; Galetta, Steven; Berger, Jeffrey
title: Hemorrhagic stroke and anticoagulation in COVID-19
date: 2020-05-23
journal: J Stroke Cerebrovasc Dis
DOI: 10.1016/j.jstrokecerebrovasdis.2020.104984
sha: 7910866f717588c2d63ddfcb11e305e8e2006b44
doc_id: 839051
cord_uid: tr58peem

Abstract Background and Purpose : Patients with the Coronavirus Disease of 2019 (COVID-19) are at increased risk for thrombotic events and mortality. Various anticoagulation regimens are now being considered for these patients. Anticoagulation is known to increase the risk for adverse bleeding events, of which intracranial hemorrhage (ICH) is one of the most feared. We present a retrospective study of 33 patients positive for COVID-19 with neuroimaging-documented ICH and examine anticoagulation use in this population. Methods : Patients over the age of 18 with confirmed COVID-19 and radiographic evidence of ICH were included in this study. Evidence of hemorrhage was confirmed and categorized by a fellowship trained neuroradiologist. Electronic health records were analyzed for patient information including demographic data, medical history, hospital course, laboratory values, and medications. Results : We identified 33 COVID-19 positive patients with ICH, mean age 61.6 years (range 37 to 83 years), 21.2% of whom were female. Parenchymal hemorrhages with mass effect and herniation occurred in 5 (15.2%) patients, with a 100% mortality rate. Of the remaining 28 patients with ICH, 7 (25%) had punctate hemorrhages, 17 (60.7%) had small- moderate size hemorrhages, and 4 (14.3%) had a large single site of hemorrhage without evidence of herniation. Almost all patients received either therapeutic dose anticoagulation (in 22 [66.7%] patients) or prophylactic dose (in 3 [9.1] patients) prior to ICH discovery. Conclusions : Anticoagulation therapy may be considered in patients with COVID-19 though the risk of ICH should be taken into account when developing a treatment regimen.

Recent studies have shown that patients with Coronavirus Disease of 2019 (COVID-19) are predisposed to developing thrombotic events (1) (2) (3) . COVID-19 patients in intensive care units (ICU) have an increased rate of venous thromboembolism (VTE), ranging from 17 to 25% (1, 2) . Moreover, COVID-19 patients have elevated coagulation markers such as D-dimer, which in turn is correlated with increased mortality (3) . Recent expert opinion recommends that all admitted patients receive VTE prophylaxis, but some centers have escalated their anticoagulation regimen for patients with certain risk factors (4) . Some ICU centers have also begun to empirically use therapeutic anticoagulation for presumed pulmonary emboli (4) .

The greatest concern of increased anticoagulation use is an increased risk of bleeding in general and of intracranial hemorrhage (ICH) in particular. In studies of patients on oral anticoagulation, ICH was shown to be the most devastating adverse event overall; these patients also had more extensive bleeding and increased mortality compared to patients with spontaneous ICH (5, 6) .

While information on bleeding remains limited in COVID-19 patients, one study suggested that many COVID-19 patients with high risk of thrombosis were simultaneously at increased risk for bleeding (7) . Although there have been recent publications about ischemic stroke in COVID-19 patients (1), literature regarding ICH in patients with COVID-19 is currently limited (8, 9) . We evaluated the presence of ICH in hospitalized COVID-19 patients and correlated imaging findings with their anticoagulation status.

This cohort study was approved by the Institutional Review Board with informed consent waived. Out of 3824 COVID-19 positive adult (age over 18) patients admitted to the NYU Langone Health system (Tisch Hospital, Kimmel Pavilion, NYU Brooklyn, NYU Winthrop, or NYU Langone Orthopedic Hospital) between March 1st and April 27th, 2020, neuroimaging was done in 755 patients. After reviewing the neuroimaging reports for these patients, 37 were found to have documented radiographic evidence of hemorrhage.

Neuroimaging for these patients was reviewed by a fellowship-trained neuroradiologist, blinded to clinical data and outcome, to verify the presence and type of hemorrhage. Four patients who had hemorrhage secondary to trauma (n=2), bleeding in brain metastases (n=1), or after tumor resection (n=1) were excluded. Of the 33 remaining patients (4.4% of the 755 patients with COVID-19 diagnoses and neuroimaging), 24 had only a CT scan and 9 had both a CT and an MRI.

Electronic health records of all patients with verified hemorrhage were then examined in order to review demographic data, medical history, hospital course, medications, and laboratory values including estimated glomerular filtration rate (eGFR) due to associations between impaired renal function and increased risk of venous thromboembolism as well as bleeding. Therapeutic anticoagulation for our cohort was classified as any intravenous heparin, any intravenous argatroban, or enoxaparin dose above prophylactic levels (40mg subcutaneously daily or 30mg subcutaneously twice daily for BMI <40; 40mg subcutaneously twice daily for BMI>40) (10, 11) . The closest D-dimer to the scan within 48 hours of imaging was recorded. Follow-up was performed through May 6 th , 2020 to track mortality, continued hospitalization, or discharge for all patients.

A modified version of the classification system used for the European Cooperative Acute Stroke Study was used to classify hemorrhages as infarct with petechial hemorrhage, infarct with small hemorrhage (<5 cm), single site of large parenchymal hemorrhage with local mass effect but without herniation, and multiple sites of parenchymal hemorrhages with mass effect and herniation ( Figure 1 ) (12) . ICH Score was calculated for all patients (13) .

We identified 33 COVID-19 positive patients with ICH, mean age 61.6 years (range 37 to 83 years), 21.2% were female, with a median ICH score of 2 (interquartile range [IQR] 1-2) ( Table   1 ). As of May 6 th , 2020, mortality occurred in 14 (42.4%) patients, 15 (45.5%) patients were still hospitalized, and 4 (12.1%) patients had been discharged. Initial radiographic evidence of hemorrhage was seen on median hospital day 17 (IQR 8-23) although 4 (12.1%) patients were found to have ICH on initial presentation. Immediately prior to discovery of the bleed, 10 (30.3%) patients had an estimated glomerular filtration rate (eGFR) below 30 mL/min/1.73 m 2 .

Within the 72 hours prior to hemorrhage discovery, 11 (33.3%) patients were thrombocytopenic with platelet counts below 150 x10 3 /μ. The median D-dimer value prior to hemorrhage discovery was 2204 ng/mL (IQR 1232-3074 ng/mL).

Therapeutic dose anticoagulation prior to ICH discovery was administered to 22 (66.7%) patients (Table 2 ). Prophylactic dose anticoagulation was administered to 3 (9.1%) patients. Two (6.1%) patients who presented with hemorrhage had been on long-term warfarin and dabigatran at home prior to admission. Six (18.2%) patients never received anticoagulation either before or during their hospitalization; three were on antiplatelet medication only, two had thrombocytopenia (platelet count <75 on admission), and a sixth presented with systemic hemorrhage of unknown etiology and thus anticoagulation was withheld. Six (27.3%) patients received concurrent inpatient therapeutic anticoagulation and antiplatelet therapy, and one (4.5%) patient received concurrent inpatient prophylactic anticoagulation and antiplatelet therapy.

Of the 22 patients that were on therapeutic anticoagulation as an inpatient, the indication in 18 (81.8%) patients was elevated D-dimer levels (median 3493 ng/mL, IQR 2468-9296 ng/ml), and 4 (18.2%) had a known or suspected thrombus (Table 2) . For these 22 patients, the therapeutic anticoagulation regimen was as follows: 15 (68.2%) received only intravenous unfractionated heparin (UFH), 3 (13.6%) received UFH and enoxaparin at different times, 3 (13.6%) received UFH and argatroban at different times, and 1 (4.5%) received only enoxaparin. Changes between UFH and enoxaparin and vice versa were made based on eGFR. Argatroban was used when there was concern for heparin-induced thrombocytopenia (HIT); however, four patients were tested for HIT antibodies, and all were eventually noted to be negative. Of the 22 patients on therapeutic anticoagulation, 12 (54.5%) had a supratherapeutic anti-factor Xa or partial thromboplastin time (PTT) within 72 hours prior to the ICH.

Of the 33 patients with ICH, 5 (15.2%) had parenchymal hemorrhages with mass effect and herniation. These images were particularly notable as all 5 patients also had radiographic evidence of diffuse hypoxic ischemic injury and brain swelling and a 100% mortality rate ( Table   1 ). All 5 patients had received therapeutic anticoagulation, 3 (60%) for a high D-dimer and 2 (40%) for a known thrombus. Imaging evidence of hemorrhage was seen on median day 22 (IQR 19-28) of hospitalization. Among these 5 patients, 4 (80%) patients had an anti-factor Xa or PTT above the upper limit of normal within 72 hours prior to the bleed ( Table 2 ). Based on review by the study neuroradiologist, all of these hemorrhages were thought to be primary ICH rather than hemorrhagic conversion of ischemic stroke.

Of the other 28 patients with ICH, 7 (25%) had punctate hemorrhages, mostly involving the cortex, 17 (60.7%) had small hemorrhages, and 4 (14.3%) had a large single site of hemorrhage without evidence of herniation (Table 1 ). Based on review by the study neuroradiologist, 26/28 (92.9%) bleeds were considered to have suffered hemorrhagic conversion of an ischemic infarct.

Mortality was 8/24 (33.3%) of the patients with punctate and small hemorrhages and 1/4 (25%) of the patients with large single hemorrhages without herniation.

Discussions regarding anticoagulation for COVID-19 patients have been intensifying as evidence of hypercoagulability in this population continues to accumulate. Decisions about anticoagulation must, in part, take the risk of ICH following anticoagulation into consideration.

Our data will certainly be helpful in this regard. We found that 4. Of particular interest is our subgroup of 5 patients with large parenchymal hemorrhages causing mass effect and herniation. Mortality was 100% in these patients, all of whom were on continuous UFH and were found to have hemorrhages many days into their hospitalization.

Although two of these patients were placed on therapeutic anticoagulation due to known or suspected thrombosis, the other three were started on therapeutic anticoagulation because of increasing D-dimer levels. Although empiric anticoagulation has been shown to lower 28-day mortality in COVID-19 patients with severely elevated D-dimer (14) , this sobering outcome underscores the need for randomized clinical trials to properly assess benefit versus risk regarding anticoagulation strategies in COVID-19. It also raises the question of whether a screening head CT should be done prior to starting anticoagulation in patients with mental status too impaired to obtain a good neurological assessment, so as to avoid the risk of catastrophic hemorrhage in an unsuspected large acute infarct.

In our study, many patients had punctate hemorrhages that were characterized as cortical in nature on MRI, but that were either mischaracterized as subarachnoid hemorrhage or not seen on CT. MRI is known to have better sensitivity than CT for detecting small ICH (15), but as neuroimaging use, and particularly MRI use, has decreased significantly during the COVID-19

pandemic, some patients with ICH may have an ICH that is diagnosed late or missed entirely.

Our study has multiple limitations, most importantly its descriptive nature as well as a small sample size. It is possible that additional patients with ICH in this cohort were not identified either because the patients were heavily sedated and there was no opportunity for a detailed neurological examination and there was a desire to limit transport out of the room for neuroimaging. As such, MRI use was limited in this cohort and adjudication of ICH etiology were made to the best of our ability. We were not able to review all COVID-19 patients getting anticoagulation to see how many of them had ICH, and we did not include patients with neuroimaging but no hemorrhage in this descriptive paper. We did not compare our patients to COVID-19 patients who had neuroimaging without evidence of hemorrhage.

Nevertheless, we believe our study provides important initial data regarding ICH and anticoagulation in patients hospitalized with COVID-19. Future work must look more deeply into the benefits and consequences of anticoagulation for COVID-19 patients, through outcomes analysis and well-powered, prospective, randomized clinical trials. Data is presented as n (%) unless otherwise specified.

*Therapeutic dose numbers sum to more than the number of patients receiving therapeutic anticoagulation as patients received multiple types of therapeutic anticoagulation at different periods of their hospitalization. 

Incidence of thrombotic complications in critically ill ICU patients with COVID-19

Prevalence of venous thromboembolism in patients with severe novel coronavirus pneumonia

Clinical course and risk factors for mortality of adult inpatients with COVID-19 in Wuhan, China: a retrospective cohort study

COVID-19 and its implications for thrombosis and anticoagulation

Early Clinical and Radiological Course, Management, and Outcome of Intracerebral Hemorrhage Related to New Oral Anticoagulants

Warfarin-associated intracerebral hemorrhage is increasing in prevalence in the United States

Attention should be paid to venous thromboembolism prophylaxis in the management of COVID-19

COVID-19 and intracerebral haemorrhage: causative or coincidental? New microbes and new infections 2020

Three unsuspected CT diagnoses of COVID-19

Enoxaparin Dosing for Venous Thromboembolism Prophylaxis in Low Body Weight Patients

Risk factors for severe hemorrhagic transformation in ischemic stroke patients treated with recombinant tissue plasminogen activator: a secondary analysis of the European-Australasian Acute Stroke Study (ECASS II)

The ICH score: a simple, reliable grading scale for intracerebral hemorrhage

Anticoagulant treatment is associated with decreased mortality in severe coronavirus disease 2019 patients with coagulopathy

Imaging of Intracranial Hemorrhage

We would like to acknowledge the NYU Family Connect Program as well as the thousands of front-line healthcare workers as an inspiration for this project.

R. Jain is a consultant for Cancer Panels Inc., receive royalties from Thieme Inc., and is on the advisory board for Nuevozen Inc. S. Galetta has served as a consultant to Biogen. The other authors report no conflicts.