CP_COVID-19: Convalescent Plasma in the Treatment of Covid-19
Study Details
Study Description
Brief Summary
This study investigates the possible adverse effects and effectiveness of convalescent plasma for patients infected with SARS-CoV-2. Following provision of informed consent, patients will be randomized into three groups: High-titre convalescent plasma, low-titre convalescent plasma or placebo. Primary outcomes of the study will cover safety and either intubation or initiation of systemic corticosteroids. Safety information collected will include serious adverse events judged to be related to administration of convalescent plasma. Microbiological and other laboratory parameters will be followed up.
Condition or Disease | Intervention/Treatment | Phase |
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Phase 2 |
Detailed Description
SARS-CoV-2 pandemic presents a serious global public health threat urgently requiring both prophylactic and therapeutic interventions. The entry of SARS-CoV-2 into human cells involves a binding between its spike protein's receptor-binding domain (RBD) and angiotensin-converting enzyme 2 (ACE2) receptor on human cells. Convalescent sera of Covid-19 patients have been shown to contain SARS-CoV-2-neutralizing antibodies. Accordingly, recovered patients are presumed to be immune to re-infection. Use of convalescent plasma as treatment warrants research, which is supported by the European Commission. Convalescent plasma (CP) therapy is a classical adaptive immunotherapy. It has been applied to prevention and treatment of various infectious diseases: evidence of success has been accumulated e.g. on treatment of SARS, MERS, and 2009 H1N1, for which satisfactory efficacy and safety have been shown.
The investigators will select as donors for CP therapy patients recovered from Covid-19 with a high neutralizing antibody titre who meet normal blood donor eligibility criteria. The donors will be recruited among participants of ongoing Covid-19 immunity studies (Clin-Covid, Commun-Covid) and/or from Finnish Red Cross Blood Service (FRCBS) blood donors.
CP will be prepared from the blood of eligible donors at the FRCBS according to previous protocols and the European guidelines for fresh frozen plasma. After the screening test results required for product release (HCV, HBV, HIV, ABO, Syphilis) are available, the units will be released. All donors will be screened for type-I-Interferon antibodies and women will be screened for HLA-antibodies. The units will be labelled with convalescence plasma labels including ICCBBA/ISBT compliant product codes. The plasma units will be frozen to -25°C within 6 hours from collection. Prior to freezing 3 ml of CP will be separated and divided in 3 aliquots to be stored, for possible later analysis.
Patients admitted to ward at HUH will be randomized 1:1:1 into three groups which will be given 1) high-titre convalescent plasma (HCP), 2) low-titre convalescent plasma (LCP) or 3) placebo. The plasma preparations and placebo will be given as one 200 mL infusion. ABORh blood group will be determined from patients prior to transfusion according to normal transfusion protocols of the hospital. The study will be double-blinded with saline as placebo given to groups three. The primary outcomes of the study will cover safety and intubation/initiation of systemic corticosteroids. AEs will be reviewed, recorded and reported up to 6 hours after administration of CP or placebo. Thromboembolic and cardiovascular events will be recorded as AEs or SAEs up to 7 days after administration of CP / placebo. SAEs will be reviewed, recorded and reported up to 7 days after administration of CP / placebo. In case of respiratory failures classified as SAEs, the reporting period is only up to 12 hours after administration of CP / placebo.
Study Design
Arms and Interventions
Arm | Intervention/Treatment |
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Experimental: High-titre CP 200mL high-titre CP on admittance |
Biological: Convalescent plasma from COVID-19 donors
Convalescent plasma from COVID-19 donors
|
Active Comparator: low-titre CP 200ml low-titre CP on admittance |
Biological: Convalescent plasma from COVID-19 donors
Convalescent plasma from COVID-19 donors
|
Placebo Comparator: Placebo 200mL saline as placebo on admittance |
Biological: Placebo
200mL saline
|
Outcome Measures
Primary Outcome Measures
- Safety (SAE) [SAEs will be reviewed, recorded and reported up to 6 hours after administration of CP or placebo.]
Immediate serious adverse events (SAE) between active and non-active group
- Safety (SAE) [SAEs will be recorded and reported up to 7 days after administration of CP or placebo.]
Subsequent serious adverse events (SAE) between active and non-active group
- Rate of intubation or systemic corticosteroids initiation [21 days post transfusion]
Intubation or systemic corticosteroid treatment (e.g. dexamethasone) started for aggravation of Covid-19
Secondary Outcome Measures
- Hospital stay [Through study completion, up to 1 year]
Number of days at hospital during the COVID-19 infection hospital period
- Mortality [Through study completion, up to 1 year]
Proportion of fatal cases during the COVID-19 infection hospital period
- Mortality [21 days post transfusion]
Proportion of fatal cases during the COVID-19 infection hospital period
- ICU stay [Within 21 days post transfusion]
Number of ICU days during the COVID-19 infection hospital period
- Ventilator days [Within 21 days post transfusion]
Number of ventilator days during the COVID-19 infection hospital period
- Severity of respiratory failure [21 days post transfusion]
Highest severity of respiratory failure using adapted WHO Clinical Progression Scale
- Viral load [During hospitalizaation, through study completion, up to 1 year]
Analyses of respiratory tract secretions by SARS-CoV-2 PCR during the COVID-19 infection hospital period
- Antibody measurements [Through study completion, up to 1 year]
Analyses of SARS-CoV-2-specific antibodies in serum and excretions
- Thrombotic complication [Through study completion, up to 1 year]
Development of a thrombotic complication, including VTE or arterial thrombosis
- The rate of participants presenting with coagulopathy disorders [21 days post transfusion]
Development of sepsis-induced coagulopathy or disseminated intravascular coagulation during the COVID-19 infection hospital period
- Number of participants with laboratory change [Through study completion, up to 1 year]
Change in inflammatory (CRP, Ferritin) and coagulopathy (P -APTT, P -AT3, P -Fibr, P -FiDD, P -FVIII., P -Trombai ja P -TT) markers during the COVID-19 infection hospital period
- Adverse effects [Through study completion, up to 1 year]
Comparison of adverse events between active and non-active group
- Convalescent plasma efficacy [21 day post transfusion]
Convalescent plasma (high or low titer) efficacy versus placebo: rate of intubation or initiating systemic corticosteroids during the COVID-19 infection hospital period
- Convalescent plasma high vs low titer efficacy [21 day post transfusion]
Comparison of efficacy of high titer CP to low titer CP: Rate of intubation or initiating systemic corticosteroids during the COVID-19 infection hospital period
- Convalescent plasma efficacy according to donor status [21 day post transfusion]
Comparison of efficacy CP obtained from vaccinated donors versus non-vaccinated donors: Rate of intubation or initiating systemic corticosteroids during the COVID-19 infection hospital period
Eligibility Criteria
Criteria
Inclusion Criteria:
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Acute Covid-19 disease at the time of recruitment laboratory-confirmed by upper respiratory tract PCR
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Patient recently (0-4 days earlier) admitted to hospital due to Covid-19 infection
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Symptom onset 10 days before recruitment (if symptom onset unknown the duration is calculated from positive PCR-test)
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the day should be recorded from the duration of the Covid-19 symptoms/positive test result
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The dose of LMWH thromboprofylaxis should be recorded
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Written informed consent.
Exclusion Criteria:
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Chronic (longer than 14 days) administration of immunosuppressants or other immune-modifying drugs within 6 months before the first dose of IMP; oral corticosteroids in dosages of ≥0.5 mg/kg/d prednisolone or equivalent are excluded ( inhaled or topical steroids allowed)
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Regular (daily), systemic administration of corticosteroids at the time on inclusion (inhaled or topical corticosteroids are allowed)
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Any confirmed or suspected immunosuppressive or immunodeficient condition, including human immunodeficiency virus (HIV) infection.
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Pregnancy or lactation.
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Alcohol or drug abuse.
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Suspected non-compliance.
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Presence of VTE, including pulmonary embolism or other manifestations of thrombosis
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Use of any investigational drug (other than hydroxychloroquine) or vaccine within 30 days prior to first dose of study vaccine or planned use during study period.
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Any clinically significant history of known or suspected anaphylaxis or hypersensitivity reaction as judged by investigator.
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Known immunoglobulin A (IgA) deficiency
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Existing treatment limitations: do-not-resuscitate (DNR) order or withholding treatment in ICU
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Any other criteria which, as judged by investigator, might compromise a patient's well-being or ability to participate in the study or its outcome.
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Active malignant disease
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CP not available for patients blood type
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Patient cannot assign written consent
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No personnel available for CP of placebo transfusion
Contacts and Locations
Locations
Site | City | State | Country | Postal Code | |
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1 | Helsinki University Central Hospital | Helsinki | Uusimaa | Finland | 00270 |
Sponsors and Collaborators
- Helsinki University Central Hospital
- Finnish Red Cross
Investigators
- Principal Investigator: Anu Kantele, MD,Prof, Helsinki University Central Hospital
Study Documents (Full-Text)
None provided.More Information
Publications
None provided.- Plasma_Covid-19