Clincosm LogoSign in Get a demo

ASCOT ADAPT: Australasian COVID-19 Trial (ASCOT) ADAptive Platform Trial

Sponsor
University of Melbourne (Other)
Overall Status
Recruiting
CT.gov ID
NCT04483960
Collaborator
The Peter Doherty Institute for Infection and Immunity (Other), Australasian Society for Infectious Diseases (Other), Middlemore Clinical Trials (Other), The George Institute (Other), Hunter Medical Research Institute (Other), The University of Queensland (Other)
2,400
Enrollment
61
Locations
7
Arms
53.1
Anticipated Duration (Months)
39.3
Patients Per Site
0.7
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

An International Multi-Centre Randomised Adaptive Platform Clinical Trial to Assess the Clinical, Virological and Immunological Outcomes in Patients with SARS-CoV-2 Infection (COVID-19).

Condition or Disease Intervention/Treatment Phase
Phase 3

Detailed Description

ASCOT is an investigator-initiated, multi-centre, open-label, randomised controlled adaptive platform trial. The study design will allow harmonisation with existing frameworks such as the Sentinel Travellers Research Preparedness Platform for Emerging Infectious Diseases (SETREP-ID) and the Randomised, embedded, multifactorial adaptive platform trial for community acquired pneumonia (REMAP-CAP) study.

Platform trials allow multiple questions to be evaluated simultaneously and sequentially within the platform, and evaluate interaction between different treatment options, to achieve the goal of determining the optimal combination of treatments for the disease as rapidly as possible. The overarching objective of ASCOT-ADAPT is to identify the regimen (combination of interventions) associated with the highest chance of survival free of advanced respiratory support or vasopressor / inotropic support at 28 days after randomisation, in adults hospitalised with COVID-19 but not requiring ICU-level care at baseline.

In the initial implementation of the adaptive platform, recruiting sites have the option to participate in one or more of three treatment domains. Consented participants will then be able to choose whether to be enrolled into one or more available domains concurrently.

Participants will then be randomised to the corresponding interventions:
Intervention domain A (antiviral):

Participants will be randomised using response adaptive randomisation (RAR) on day 1 to receive either i) standard of care without nafamostat; or ii) standard of care with nafamostat

(Domain Closed) Intervention domain B (antibody): Participants will be randomised using response adaptive randomisation (RAR) on day 1 to receive either i) standard of care without hyperimmune globulin; or ii) standard of care with hyperimmune globulin

(Domain Closed) Intervention domain C (anticoagulation): Participants will be randomised using response adaptive randomisation (RAR) on day 1 to receive either i) standard dose thromboprophylaxis; or ii) intermediate dose thromboprophylaxis; or iii) therapeutic anticoagulation

Daily data will be collected for the first 28 days or until discharge, whichever is earlier. There will be a core dataset collected for all patients at all sites and enhanced and research data and biological samples for sites with capacity. Participants will be followed up at Day 90.

Study Design

Study Type:
Interventional
Anticipated Enrollment :
2400 participants
Allocation:
Randomized
Intervention Model:
Factorial Assignment
Intervention Model Description:
Participants enrolled into the study have the option of deciding whether to be randomised in one or more (if available) treatment domains concurrently, if they meet the eligibility criteria.Participants enrolled into the study have the option of deciding whether to be randomised in one or more (if available) treatment domains concurrently, if they meet the eligibility criteria.
Masking:
None (Open Label)
Masking Description:
This is an open-label study.
Primary Purpose:
Treatment
Official Title:
A Multi-centre Randomised Adaptive Platform Clinical Trial to Assess Clinical, Virological and Immunological Outcomes in Patients With SARS-CoV-2 Infection (COVID-19)
Actual Study Start Date :
Jul 28, 2020
Anticipated Primary Completion Date :
Dec 31, 2024
Anticipated Study Completion Date :
Dec 31, 2024

Arms and Interventions

Arm Intervention/Treatment
No Intervention: Antiviral - Standard of care

Standard of care without nafamostat mesilate
Experimental: Antiviral - nafamostat mesilate

Nafamostat continuous IV infusion for 7 days or until day of hospital discharge at a dose of 0.2mg/kg/hour. No adjustment in dose is needed for renal impairment, including for renal dialysis. The daily dose of nafamostat should be administered in 500 mL (rate of infusion 20.8 mL/hour) of normal saline. Normal saline is recommended (due to the tendency for patients with COVID-19 towards hyponatraemia) but not mandated, and 5% dextrose would be acceptable if felt clinically appropriate.

Drug: Nafamostat Mesilate
Nafamostat continuous IV infusion for 7 days or until day of hospital discharge at a dose of 0.2mg/kg/hour. No adjustment in dose is needed for renal impairment, including for renal dialysis. The daily dose of nafamostat should be administered in 500 mL (rate of infusion 20.8 mL/hour) of normal saline. Normal saline is recommended (due to the tendency for patients with COVID-19 towards hyponatraemia) but not mandated, and 5% dextrose would be acceptable if felt clinically appropriate.
Other Names:
  • Nafabelltan

    		•
    Active Comparator: (Arm Closed) Anticoagulation - standard dose thromboprophylaxis

    Patients will be administered a standard thromboprophylactic dose of low molecular weight heparin, choice of agent according to availability and local practice at the participating site.

    Drug: Enoxaparin
    Patients will be administered either a standard dose, intermediate dose or therapeutic anticoagulation of low molecular weight heparin (depending on assigned arm), choice of agent according to availability and local practice at the participating site. The maximum dose of Enoxaparin will be 1mg/kg q12h or 1.5mg/kg q24h.

    Drug: Dalteparin
    Patients will be administered either a standard dose, intermediate dose or therapeutic anticoagulation of low molecular weight heparin (depending on assigned arm), choice of agent according to availability and local practice at the participating site. The maximum dose of Dalteparin will be 100IU/kg q12h or 200IU/kg q24h.

    Drug: Tinzaparin
    Patients will be administered either a standard dose, intermediate dose or therapeutic anticoagulation of low molecular weight heparin (depending on assigned arm), choice of agent according to availability and local practice at the participating site. The maximum dose of Tinzaparin will be 175IU/kg q24h (not available within Australia).
    Experimental: (Arm Closed) Anticoagulation - intermediate dose thromboprophylaxis

    Patients will be administered an intermediate dose of low molecular weight heparin, choice of agent according to availability and local practice at the participating site. The maximum dose of enoxaparin will be 120 mg/d, tinzaparin 125 IU/kg/day (not available within Australia), and Dalteparin 15,000 IU/d.

    Drug: Enoxaparin
    Patients will be administered either a standard dose, intermediate dose or therapeutic anticoagulation of low molecular weight heparin (depending on assigned arm), choice of agent according to availability and local practice at the participating site. The maximum dose of Enoxaparin will be 1mg/kg q12h or 1.5mg/kg q24h.

    Drug: Dalteparin
    Patients will be administered either a standard dose, intermediate dose or therapeutic anticoagulation of low molecular weight heparin (depending on assigned arm), choice of agent according to availability and local practice at the participating site. The maximum dose of Dalteparin will be 100IU/kg q12h or 200IU/kg q24h.

    Drug: Tinzaparin
    Patients will be administered either a standard dose, intermediate dose or therapeutic anticoagulation of low molecular weight heparin (depending on assigned arm), choice of agent according to availability and local practice at the participating site. The maximum dose of Tinzaparin will be 175IU/kg q24h (not available within Australia).
    Experimental: (Arm Closed) Anticoagulation - therapeutic anticoagulation

    Therapeutic anticoagulation administered with LMWH daily until hospital discharge, admission to ICU or for a maximum of 28 days from randomisation. Choice of LMWH according to availability and local practice at the participating site

    Drug: Enoxaparin
    Patients will be administered either a standard dose, intermediate dose or therapeutic anticoagulation of low molecular weight heparin (depending on assigned arm), choice of agent according to availability and local practice at the participating site. The maximum dose of Enoxaparin will be 1mg/kg q12h or 1.5mg/kg q24h.

    Drug: Dalteparin
    Patients will be administered either a standard dose, intermediate dose or therapeutic anticoagulation of low molecular weight heparin (depending on assigned arm), choice of agent according to availability and local practice at the participating site. The maximum dose of Dalteparin will be 100IU/kg q12h or 200IU/kg q24h.

    Drug: Tinzaparin
    Patients will be administered either a standard dose, intermediate dose or therapeutic anticoagulation of low molecular weight heparin (depending on assigned arm), choice of agent according to availability and local practice at the participating site. The maximum dose of Tinzaparin will be 175IU/kg q24h (not available within Australia).
    No Intervention: (Arm Closed) Antibody - Standard of Care

    No hyperimmune globulin
    Experimental: (Arm Closed) Antibody - hyperimmune globulin

    2 doses of 30mL (3x10mL vials) of COVID-19 Hyper-Immunoglobulin (Human) given over 2 days within 48 hours of randomisation

    Biological: Hyperimmune globulin
    2 doses of 30mL (3x10mL vials) of COVID-19 Hyper-Immunoglobulin (Human) given over 2 days within 48 hours of randomisation. Three vials will have approximately 10500 AU of neutralising antibodies, equivalent to approximately 200mL of convalescent plasma

    Outcome Measures

    Primary Outcome Measures

    1. Death from any cause or requirement of new intensive respiratory support (invasive or non-invasive ventilation) or vasopressor/inotropic support. [28 days]

      This includes any participant who receives non-invasive mechanical ventilation (either CPAP or BIPAP, apart from the below considerations) any time after enrolment even if not transferred to ICU. It does NOT include the use of humidified high-flow nasal prong oxygen. Participants on pre-existing home BiPAP or CPAP will not be considered to have met the primary outcome unless they have either i. required invasive mechanical ventilation (i.e. intubation), or ii. graduated from CPAP only whilst asleep to BiPAP at any time, or iii. graduated from BiPAP only whilst asleep to BiPAP for >12 hours/day, or iv. died by day 28

    Secondary Outcome Measures

    1. Time to clinical recovery [28 days]

      Defined as the first day, during the 28 days after enrolment, on which a patient satisfies categories 1, 2, or 3 on the WHO eight-point ordinal outcome scale. For the purposes of this outcome measure, it will be assumed that the participant is not hospitalised on the first day following discharge.

    2. WHO 8-point ordinal outcome scale [28 days]

      The ordinal score is: Not hospitalised, no limitations on activities Not hospitalised, limitation on activities Hospitalised, not requiring supplemental oxygen and no longer requiring ongoing medical care (used if hospitalization was extended for infection control purposes) Hospitalised, not requiring supplemental oxygen but requiring ongoing medical care (COVID-19 related or other medical conditions) Hospitalised, requiring supplemental oxygen Hospitalised, on non-invasive ventilation or high flow oxygen devices Hospitalised, on invasive mechanical ventilation or ECMO Death. Admission to a Hospital in the Home unit is not counted as hospitalisation for the purposes of this ordinal scale. Patients who have been admitted to hospital and transferred to a Hospital in the Home unit will be assessed as either ordinal score 1 or 2.

    3. All-cause mortality [28 days and 90 days]

      All-cause mortality

    4. Days alive and free of hospital [28 days]

      Number of days Days spent in a Hospital in the Home unit will not be counted as days in hospital as hospital means 'acute-care hospital' for the purposes of this endpoint.

    5. Days alive and free of invasive or non-invasive ventilation [28 days]

      Number of days

    6. Shortness of breath [28 days and 90 days]

      Patient reported outcome. Dichotomous comparison of a subjective measure of shortness of breath such as: "Are you currently experiencing shortness of breath that you didn't have before you got COVID, or which is worse now than before you got COVID?" Ordinal comparison of the modified Medical Research Council (mMRC) breathlessness scale: Modified Medical Research Council (mMRC) Dyspnoea Scale for grading the severity of breathlessness during daily activities: 0 - I only get breathless with strenuous exercise - I get short of breath when hurrying on level ground or walking up a slight hill - On level ground, I walk slower than people of the same age because of breathlessness, or I have to stop for breath when walking at my own pace on the level - I stop for breath after walking about 100 metres or after a few minutes on level ground - I am too breathless to leave the house or I am breathless when dressing or undressing

    7. Quality of life [28 days and 90 days]

      Measured by the EQ-5D-5L questionnaire

    8. Antiviral domain-specific outcome: Viral clearance [3 and 7 days]

      Proportion of patients with negative SARS-CoV-2 RT-PCR from upper or lower respiratory tract samples, for those with results available.

    9. Antiviral domain-specific outcome: Viral load [3 and 7 days]

      Changes in cycle threshold value in RT-PCR for SARS-CoV-2 from baseline to day 3 and from baseline to day 7, for those with results available from the same respiratory tract sample type.

    10. Antiviral domain-specific outcome: Safety (Liver enzymes) [Up to day 28 or day of discharge from hospital, whichever is earlier]

      o Elevation of Alanine Transaminase (ALT) or Aspartate Transaminase (AST) to >5x upper limit of normal

    11. Antiviral domain-specific outcome: Safety (potassium) [Up to day 28 or day of discharge from hospital, whichever is earlier]

      o Elevation of serum potassium to >5.5 mmol/L

    12. Antiviral domain-specific outcome: Safety (sodium) [Up to day 28 or day of discharge from hospital, whichever is earlier]

      o Decrease of serum sodium to <125 mmol/L

    13. Antiviral domain-specific outcome: Safety (bleeding) [Up to day 28 or day of discharge from hospital, whichever is earlier]

      o Major bleeding as defined by the International Society on Thrombosis and Haemostasis (ISTH).

    14. Antiviral domain-specific outcome: Safety (thrombophlebitis) [Up to day 28 or day of discharge from hospital, whichever is earlier]

      o Thrombophlebitis/vasculitis at IV line site

    15. Antiviral domain-specific outcome: serious adverse reactions [28 days]

      Any safety event that, in the judgment of the investigator, is both serious and either possibly, probably or definitely related to the study intervention(s).

    16. Anticoagulation domain-specific outcome: Confirmed deep venous thrombosis [28 days]

      Yes/No

    17. Anticoagulation domain-specific outcome: Confirmed pulmonary embolus [28 days]

      Yes/No

    18. Anticoagulation domain-specific outcome: Confirmed acute myocardial infarction [28 days]

      Yes/No

    19. Anticoagulation domain-specific outcome: Confirmed ischemic cerebrovascular event [28 days]

      Yes/No

    20. Anticoagulation domain-specific outcome: Major bleeding [28 days]

      Yes/No - As defined by International Society on Thrombosis and Haemostasis (ISTH). Site of bleeding and which of the ISTH criteria are met will be recorded.

    21. Anticoagulation domain-specific outcome: Clinically relevant non-major bleeding [28 days]

      Yes/No - As defined by International Society on Thrombosis and Haemostasis (ISTH).

    22. Anticoagulation domain-specific outcome: Heparin-induced thrombocytopenia (HIT) [28 days]

      Yes/No - During index hospitalisation

    23. Anticoagulation domain-specific outcome: Other confirmed thrombotic event [28 days]

      Yes/No - During index hospitalisation

    24. Antibody domain-specific outcome: Serious treatment-related adverse events [Within 24 hours of treatment]

      Including: Serious allergic reaction or anaphylaxis Transfusion-related acute lung injury (TRALI)

    25. Antibody domain-specific outcome: Haemolysis [Within 72 hours of last transfusion]

      Yes/No

    26. Antibody domain-specific outcome: Confirmed arterial thrombosis [28 days]

      Yes/No - acute myocardial infarction, ischaemic cerebrovascular event, other

    27. Antibody domain-specific outcome: Confirmed venous thrombosis [28 days]

      Yes/No - deep vein thrombosis, pulmonary embolus, other

    Eligibility Criteria

    Criteria

    Ages Eligible for Study:
    18 Years and Older
    Sexes Eligible for Study:
    All
    Accepts Healthy Volunteers:
    No
    Platform Inclusion Criteria:

    1. Age ≥ 18 years

    2. Admitted to an acute-care hospital

    3. Confirmed SARS-CoV-2 by nucleic acid testing or rapid antigen testing in the 14 days prior to randomisation

    4. Able to be randomised within 14 days of symptom onset

    5. At least one symptom or sign attributable to SARS-CoV-2 infection

    Exclusion Criteria:
    A. Overall platform exclusions:

    1. Currently receiving acute intensive respiratory support (invasive or non-invasive mechanical ventilation) or vasopressor/inotropic support. Note, participants already on community based non-invasive ventilation (either CPAP or BiPAP) can still be recruited. Humidified high flow nasal oxygen will not be considered an exclusion criterion.

    2. Previous participation in the trial

    3. Treating team deems enrolment in the study is not in the best interests of the patient

    4. Death is deemed to be imminent and inevitable within the next 24 hours

    5. Either the patient or their primary treating clinician are not committed to active treatment.

    This criterion seeks to exclude those patients where supportive comfort measures only are being provided. Patients who are planned for active ward management with a clear aim to improve survival, even if intensive care unit level support is not being offered, should still be included.

    B. Domain A (Antiviral) intervention-level exclusions:
    Criteria that exclude a patient from one or more interventions are:
    Nafamostat:

    • Known current decompensated liver disease (Child-Pugh B or C)

    • The treating clinician intends to continue or commence therapeutic anticoagulation

    • A current or recurrent condition with a high risk of major bleeding (e.g. bleeding disorder), or a baseline coagulation profile (within the previous 3 days) that indicates a high risk of bleeding, that would be considered a contraindication to receive therapeutic anticoagulation

    • Serum Potassium >5.5 mmol/L (based on most recent blood test result collected as part of routine care within the previous 3 days)

    • Serum Sodium <120 mmol/L (based on most recent blood test result collected as part of routine care within the previous 3 days)

    • Hypersensitivity to nafamostat

    • Pregnancy or breastfeeding

    • Currently receiving or have received nafamostat in the past 7 days

    • Decompensated heart failure or renal dialysis and clinician believes an extra 500mL fluid/day would be detrimental There are no domain-level exclusions for the antiviral domain.

    C. Domain B (Antibody - hyperimmunoglobulin or standard care) specific exclusions:

    1. Participant has already received treatment with SARS-CoV-2-specific immunoglobulin therapy (convalescent plasma, hyperimmune globulin or monoclonal antibody) within 3 months prior to enrolment

    2. Treating team deems enrolment in antibody intervention is not in the best interests of the patient.

    3. Participant has received a SARS-COV-2 vaccine within the prior 30 days

    4. Known previous history of serious allergic reaction to blood product transfusion, intravenous immunoglobulin or other injectable form of IgG will exclude a patient from hyperimmune globulin

    5. Known personal or religious objections to receiving blood products will exclude a patient from hyperimmune globulin

    6. Pregnant or breastfeeding female participants will be excluded from hyperimmune globulin

    7. Prior history of a thrombotic event (including acute coronary syndromes, cerebrovascular syndromes, pulmonary or deep vein thrombosis) within the prior 30 days of randomisation will exclude a patient from receiving hyperimmune globulin

    8. Having a creatinine clearance of less than 50mL/min will exclude a patient from receiving hyperimmune globulin

    D. Domain C (Anticoagulation) domain-level exclusions:
    Patients will be excluded from this domain if they have any of the following:

    • Receiving dual antiplatelet therapy

    • The treating clinician intends to continue or commence therapeutic anticoagulation

    • Contraindication to receiving low molecular weight heparin or unfractionated heparin, including the known or suspected history of heparin-induced thrombocytopenia or other adverse reaction to prior heparin exposure such as hypersensitivity

    • Severe thrombocytopenia (platelet count less than 530 x 109/L)

    • History of intracranial haemorrhage in the previous 3 months

    • Severe renal impairment, defined as estimated glomerular filtration rate less than 15ml/min/1.73m2

    • A current or recurrent condition with a high risk of major bleeding (e.g. bleeding disorder), or a baseline coagulation profile (within the previous 3 days) that indicates a high risk of bleeding, that would be considered a contraindication to receive therapeutic anticoagulation

    Contacts and Locations

    Locations

    Site City State Country Postal Code
    1 Calvary Public Bruce Hospital Bruce Australian Capital Territory Australia 2617
    2 The Canberra Hospital Canberra Australian Capital Territory Australia 2605
    3 Armidale Hospital Armidale New South Wales Australia 2350
    4 Bankstown-Lidcombe Hospital Bankstown New South Wales Australia 2200
    5 Blacktown Hospital Blacktown New South Wales Australia 2148
    6 Campbelltown Hospital Campbelltown New South Wales Australia 2560
    7 Royal Prince Alfred Hospital Camperdown New South Wales Australia 2050
    8 The Sutherland Hospital Caringbah New South Wales Australia 2229
    9 Coffs Harbour Health Campus Coffs Harbour New South Wales Australia 2450
    10 St Vincent's Hospital Sydney Darlinghurst New South Wales Australia 2010
    11 Northern Beaches Hospital Frenchs Forest New South Wales Australia 2086
    12 Griffith Base Hospital Griffith New South Wales Australia 2680
    13 Hornsby Ku-Ring Gai Hospital Hornsby New South Wales Australia 2077
    14 Nepean Hospital Kingswood New South Wales Australia 2747
    15 St George Hospital Kogarah New South Wales Australia 2217
    16 Liverpool Hospital Liverpool New South Wales Australia 2170
    17 John Hunter Hospital New Lambton Heights New South Wales Australia 2305
    18 Orange Health Service Orange New South Wales Australia 2800
    19 Port Macquarie Base Hospital Port Macquarie New South Wales Australia 2444
    20 Prince of Wales Hospital Randwick New South Wales Australia 2031
    21 Royal North Shore Hospital St Leonards New South Wales Australia 2065
    22 The Tweed Hospital Tweed Heads New South Wales Australia 2485
    23 Wagga Wagga Base Hospital Wagga Wagga New South Wales Australia 2650
    24 Calvary Mater Newcastle Waratah New South Wales Australia 2298
    25 Westmead Hospital Westmead New South Wales Australia 2145
    26 Wollongong Hospital Wollongong New South Wales Australia 2500
    27 Royal Darwin Hospital Tiwi Northern Territory Australia 0810
    28 Sunshine Coast University Hospital Birtinya Queensland Australia 4575
    29 The Prince Charles Hospital Chermside Queensland Australia 4032
    30 Royal Brisbane and Women's Hospital Herston Queensland Australia 4120
    31 Gold Coast University Hospital Southport Queensland Australia 4215
    32 Lyell McEwin Hospital Elizabeth Vale South Australia Australia 5112
    33 Royal Hobart Hospital Hobart Tasmania Australia 7000
    34 Launceston General Hospital Launceston Tasmania Australia 7250
    35 Ballarat Health Services Ballarat Central Victoria Australia 3350
    36 St John of God Ballarat Hospital Ballarat Victoria Australia 3350
    37 Bendigo Health Bendigo Victoria Australia 3550
    38 Eastern Health (Box Hill Hospital) Box Hill Victoria Australia 3128
    39 Monash Health Clayton Victoria Australia 3168
    40 Northern Health Epping Victoria Australia 3076
    41 St. Vincent's Hospital Melbourne Fitzroy Victoria Australia 3065
    42 Frankston Hospital - Penninsula Health Frankston Victoria Australia 3199
    43 Peninsula Private Hospital Frankston Victoria Australia 3199
    44 Barwon Health - University Hospital Geelong Geelong Victoria Australia 3220
    45 Austin Health Heidelberg Victoria Australia 3084
    46 Cabrini Health Malvern Victoria Australia 3144
    47 Alfred Hospital Melbourne Victoria Australia 3004
    48 Royal Melbourne Hospital Parkville Victoria Australia 3050
    49 Epworth Richmond Richmond Victoria Australia 3121
    50 Goulburn Valley Health Shepparton Victoria Australia 3630
    51 Western Health St Albans Victoria Australia 3021
    52 Latrobe Regional Hospital Traralgon Victoria Australia 3844
    53 West Gippsland Hospital Warragul Victoria Australia 3820
    54 Albury Wodonga Health Wodonga Victoria Australia 3690
    55 Rockingham General Hospital Cooloongup Western Australia Australia 6168
    56 Joondalup Health Campus Joondalup Western Australia Australia 6027
    57 Armadale Health Service Mount Nasura Western Australia Australia 6112
    58 Fiona Stanley Hospita Murdoch Western Australia Australia 6150
    59 Sir Charles Gairdner Hospital Nedlands Western Australia Australia 6009
    60 Royal Perth Hospital Perth Western Australia Australia 6000
    61 St John of God Subiaco Hospital Subiaco Western Australia Australia 6008

    Sponsors and Collaborators

    • University of Melbourne
    • The Peter Doherty Institute for Infection and Immunity
    • Australasian Society for Infectious Diseases
    • Middlemore Clinical Trials
    • The George Institute
    • Hunter Medical Research Institute
    • The University of Queensland

    Investigators

    • Study Chair: Steven Tong, A/Prof, Melbourne Health

    Study Documents (Full-Text)

    None provided.

    More Information

    Publications

    None provided.
    Responsible Party:
    Associate Professor Steven Tong, Associate Professor, University of Melbourne
    ClinicalTrials.gov Identifier:
    NCT04483960
    Other Study ID Numbers:
    • ERM 62646-A
    First Posted:
    Jul 23, 2020
    Last Update Posted:
    Jul 28, 2022
    Last Verified:
    Jul 1, 2022
    Studies a U.S. FDA-regulated Drug Product:
    No
    Studies a U.S. FDA-regulated Device Product:
    No
    Product Manufactured in and Exported from the U.S.:
    No
    Additional relevant MeSH terms:
    Infections
    COVID-19
    Nafamostat
    Enoxaparin
    Dalteparin
    Tinzaparin
    Heparin, Low-Molecular-Weight

    Study Results

    No Results Posted as of Jul 28, 2022