ANTICOVID: ANTIcoagulation in Severe COVID-19 Patients
Study Details
Study Description
Brief Summary
Coronavirus disease 2019 (COVID-19), a viral respiratory illness caused by the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), may predispose patients to thrombotic disease due to a state of profound inflammation, platelet activation, and endothelial dysfunction leading to respiratory distress and increased mortality. The incidence of macrovascular thrombotic events varies from 10 to 30% in COVID-19 hospitalized patients depending on the type of arterial or vein thrombosis captured and severity of illness . Observational results in patients receiving routine low-dose prophylactic anticoagulation (LD-PA), several institutions have recently released guidance statement to prevent macrovascular thrombotic events with dose escalation anticoagulation. In these recommendations, high-dose prophylactic anticoagulation (HD-PA) and therapeutic anticoagulation (TA) can be employed either empirically or based on the body mass index and increased D-dimer values. No randomized trial has validated this approach, and other recent recommendations challenge this approach. Microvascular thrombotic events are also of major concern in critically ill patients with COVID-19, even in the absence of obvious macrovascular thrombotic events. A large review of autopsy findings in COVID-19-related deaths reported micro thrombi in small pulmonary vessels. More generally, COVID-19-induced endothelitis and coagulopathy across vascular beds of different organs lead to widespread microvascular thrombosis with microangiopathy and occlusion of capillaries. Thus, in severe COVID-19 patients requiring oxygen therapy without initial macrovascular thrombotic event, a HD-PA or a TA could be beneficial by limiting the extension of microvascular thrombosis and the evolution of the lung and multi-organ microcirculatory dysfunction. In a large observational cohort of 2,773 COVID-19 patients, a lower in-hospital mortality in ventilated patients receiving TA as compared to those receiving PA (29.1% vs. 62.7%). Our hypothesis is dual: i) first, that TA and HD-PA strategies mitigate microthrombosis and each limit the progression of COVID-19, including respiratory failure and multi-organ dysfunction, with in fine a decreased mortality and duration of disease, as compared to a low-dose PA; ii) second, that TA outperforms HD-PA in this setting.
Condition or Disease | Intervention/Treatment | Phase |
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Phase 2 |
Study Design
Arms and Interventions
Arm | Intervention/Treatment |
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Experimental: Low dose prophylactic anticoagulation LD-PA : 3500 IU/24h |
Drug: Tinzaparin, Low dose prophylactic anticoagulation
Participants randomized to the LD-PA strategie will receive the low weight molecular heparin (LMWH) tinzaparin, considering its contraindications, recommended dose ranges and monitoring if applicable, as follows: LD-PA : 3500 IU/24h.
If tinzaparin is not punctually available, the use of enoxaparin will be allowed as follows: LD-PA: 4000 IU/24h.
After day-14, or hospital discharge, or in case of an indication for TA, or of serious adverse event related to anticoagulation, the investigational anticoagulation strategy will be discontinued and anticoagulation treatment will be left at the discretion of attending physicians.
Recommendations for the management of COVID-19 pneumonia will be followed, including the use of dexamethasone. These recommendations will be subject to modifications based on the new literature data.
Other Names:
|
Experimental: High dose prophylactic anticoagulation HD-PA : 7000 IU/24h. |
Drug: Tinzaparin, High dose prophylactic anticoagulation
Participants randomized to the HD-PA strategie will receive the low weight molecular heparin (LMWH) tinzaparin, considering its contraindications, recommended dose ranges and monitoring if applicable, as follows: HD-PA : 7000 IU/24h.
If tinzaparin is not punctually available, the use of enoxaparin will be allowed as follows: HD-PA: 4000 IU/12h.
After day-14, or hospital discharge, or in case of an indication for TA, or of serious adverse event related to anticoagulation, the investigational anticoagulation strategy will be discontinued and anticoagulation treatment will be left at the discretion of attending physicians.
Recommendations for the management of COVID-19 pneumonia will be followed, including the use of dexamethasone. These recommendations will be subject to modifications based on the new literature data.
Other Names:
|
Experimental: Therapeutic anticoagulation TA : 175 IU/kg/24h. |
Drug: Tinzaparin,Therapeutic anticoagulation
Participants randomized to the TA strategie will receive the low weight molecular heparin (LMWH) tinzaparin, considering its contraindications, recommended dose ranges and monitoring if applicable, as follows: TA : 175 IU/kg/24h.
If tinzaparin is not punctually available, the use of enoxaparin will be allowed as follows: TA: 100 IU/kg/12h.
After day-14, or hospital discharge, or in case of an indication for TA, or of serious adverse event related to anticoagulation, the investigational anticoagulation strategy will be discontinued and anticoagulation treatment will be left at the discretion of attending physicians.
Recommendations for the management of COVID-19 pneumonia will be followed, including the use of dexamethasone. These recommendations will be subject to modifications based on the new literature data.
Other Names:
|
Outcome Measures
Primary Outcome Measures
- All-cause mortality [Day-28]
- Number of days to clinical improvement [Day-28]
Clinical improvement will be assessed through a seven-category ordinal scale derived from the WHO scale, using the following categories: 1. not hospitalized with resumption of normal activities; 2. not hospitalized, but unable to resume normal activities; 3. hospitalized, not requiring supplemental oxygen; 4. hospitalized, requiring supplemental oxygen; 5. hospitalized, requiring nasal high-flow oxygen therapy, noninvasive mechanical ventilation, or both; 6. hospitalized, requiring ECMO, invasive mechanical ventilation, or both; and 7. death. As all included patients will at least require oxygen supplementation, live discharge from hospital will represent a minimal 2-points decrease in the 7-points scale, thus a clinical improvement.
Secondary Outcome Measures
- Score on WHO Ordinal Scale [Day-28]
- Number of days alive and free from supplemental oxygen at Day-28 [Day-28]
- Proportion of patients needing intubation at Day-28 [Day-28]
- Number of days alive and free from invasive mechanical ventilation at Day-28 [Day-28]
- Number of days alive and free from vasopressors at Day-28 [Day-28]
- Length of intensive care unit stay [Day-28]
- Length of hospital stay [Day-28]
- Quality of life and disability at assessed using a quality of life questionnaire [Day-90]
- All-cause deaths [Day-28 and Day-90]
- Proportion of patients with at least one thrombotic event at Day-28 [Day-28]
- D-dimers [Day-7]
- Proportion of patients with at least one major bleeding event (MBE) at Day-28 [Day-28]
- Proportion of patients with at least one life-threatening bleeding event at Day-28 [Day-28]
- Proportion of patients with any bleeding event at Day-28 [Day-28]
- Proportion of patients with Heparin Induced Thrombocytopenia (HIT) at Day-28 [Day-28]
- 7-points ordinal scale [Day-28]
- Sepsis-Induced Coagulopathy Score (SCS) [Day-7]
Eligibility Criteria
Criteria
Inclusion Criteria:
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Age ≥ 18 years ;
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Severe COVID-19 pneumonia, defined by:
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A newly-appeared pulmonary parenchymal infiltrate; AND
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a positive RT-PCR (either upper or lower respiratory tract) for COVID-19 (SARS-CoV-2); AND
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WHO progression scale ≥ 5
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Written informed consent (patient, next of skin or emergency situation).
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In view of the exceptional and urgent situation, affiliation to a social security scheme will not be a criterion for inclusion.
Exclusion Criteria:
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Pregnancy and breast feeding woman;
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Postpartum (6 weeks);
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Extreme weights (<40 kg or >100 kg);
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Patients admitted since more than 72 hours to the hospital (if the WHO ordinal scale is 5 at time of inclusion) or since more than 72 hours to the intensive care unit (if the WHO ordinal scale is 6 or more at time of inclusion);
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Need for therapeutic anticoagulation (except for COVID-related pulmonary thrombosis);
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Bleeding event related to hemostasis disorders, acute clinically significant bleed, current gastrointestinal ulcer or any organic lesion with high risk for bleeding
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Platelet count < 50 G/L;
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Within 15 days of recent surgery, within 24 hours of spinal or epidural anesthesia;
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Any prior intracranial hemorrhage, enlarged acute ischemic stroke, known intracranial malformation or neoplasm, acute infectious endocarditis;
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Severe renal failure (creatinine clearance <30 mL/min);
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Iodine allergy;
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Hypersensitivity to heparin or its derivatives including low-molecular-weight heparin;
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History of type II heparin-induced thrombocytopenia;
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Chronic oxygen supplementation;
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Moribund patient or death expected from underlying disease during the current admission;
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Patient deprived of liberty and persons subject to institutional psychiatric care;
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Patients under guardianship or curatorship;
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Participation to another interventional research on anticoagulation.
Contacts and Locations
Locations
Site | City | State | Country | Postal Code | |
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1 | Henri Mondor Hospital | Créteil | France | 94000 |
Sponsors and Collaborators
- Assistance Publique - Hôpitaux de Paris
Investigators
- Study Director: Vincent LABBE, MD, Assistance Publique Hopitaux de Paris (AP-HP)
Study Documents (Full-Text)
None provided.More Information
Publications
None provided.- APHP201624
- 2020-A03531-38