Covid 19 Research using Clinical Trials (Home Page)
Convalescent plasmaWiki
Developed by Shray Alag
Clinical Trial MeSH HPO Drug Gene SNP Protein Mutation
Correlated Drug Terms (42)
| Name (Synonyms) | Correlation | |
|---|---|---|
| drug2910 | nasopharyngeal Covid 19 RT-PCR Wiki | 0.25 |
| drug1425 | Macrolide administered for up to 14 days Wiki | 0.25 |
| drug223 | Assessing impact of COVID19 Wiki | 0.25 |
| drug2021 | Radspherin Wiki | 0.25 |
| drug2735 | allogeneic human dental pulp stem cells (BSH BTC & Utooth BTC) Wiki | 0.25 |
| drug1227 | Interferon-β1a Wiki | 0.25 |
| drug1424 | Macrolide administered for 3-5 days Wiki | 0.25 |
| drug2705 | YH25448 Wiki | 0.25 |
| drug949 | Fixed-duration Hydrocortisone Wiki | 0.25 |
| drug1932 | Protocolised mechanical ventilation strategy Wiki | 0.25 |
| drug1085 | Hydroxychloroquin with Azithromycin Wiki | 0.25 |
| drug2254 | Shock-dependent hydrocortisone Wiki | 0.25 |
| drug1092 | Hydroxychloroquine + lopinavir/ritonavir Wiki | 0.25 |
| drug476 | COVID-19 exposure Wiki | 0.25 |
| drug1820 | Piperacillin-tazobactam Wiki | 0.25 |
| drug1240 | Intervention group_rehabilitation program Wiki | 0.25 |
| drug156 | Amoxicillin-clavulanate Wiki | 0.25 |
| drug999 | Global Longitudinal Strain Wiki | 0.25 |
| drug950 | Fixed-duration higher dose Hydrocortisone Wiki | 0.25 |
| drug532 | Ceftriaxone Wiki | 0.25 |
| drug1253 | Intravenous saline injection (Placebo) Wiki | 0.25 |
| drug946 | Five-days oseltamivir Wiki | 0.25 |
| drug1523 | Moxifloxacin or Levofloxacin Wiki | 0.25 |
| drug531 | Ceftaroline Wiki | 0.25 |
| drug2234 | Serological screening for IgG and IgM antibodies against COVID-19 Wiki | 0.25 |
| drug2194 | Sampling of tissue Wiki | 0.25 |
| drug2472 | Ten-days oseltamivir Wiki | 0.25 |
| drug2499 | Therapeutic anticoagulation Wiki | 0.18 |
| drug2263 | Simvastatin Wiki | 0.18 |
| drug1893 | Prazosin Wiki | 0.18 |
| drug670 | Corticosteroid Wiki | 0.18 |
| drug1365 | Lopinavir-Ritonavir Wiki | 0.18 |
| drug2994 | self-administered questionnaire Wiki | 0.14 |
| drug2326 | Standard of care Wiki | 0.11 |
| drug2197 | Sarilumab Wiki | 0.11 |
| drug159 | Anakinra Wiki | 0.09 |
| drug2527 | Tocilizumab Wiki | 0.09 |
| drug1372 | Lopinavir/ritonavir Wiki | 0.08 |
| drug2662 | Vitamin C Wiki | 0.08 |
| drug1086 | Hydroxychloroquine Wiki | 0.05 |
| drug262 | Azithromycin Wiki | 0.04 |
| drug1822 | Placebo Wiki | 0.01 |
Correlated MeSH Terms (18)
| Name (Synonyms) | Correlation | |
|---|---|---|
| D009202 | Cardiomyopathies NIH | 0.29 |
| D002289 | Carcinoma, Non-Small-Cell Lung NIH | 0.25 |
| D000077216 | Carcinoma, Ovarian Epithelial NIH | 0.25 |
| D006819 | Hyaline Membrane Disease NIH | 0.25 |
| D010534 | Peritoneal Neoplasms NIH | 0.25 |
| D006528 | Carcinoma, Hepatocellular NIH | 0.25 |
| D002277 | Carcinoma NIH | 0.22 |
| D003289 | Convalescence NIH | 0.22 |
| D010051 | Ovarian Neoplasms NIH | 0.18 |
| D045169 | Severe Acute Respiratory Syndrome NIH | 0.06 |
| D002318 | Cardiovascular Diseases NIH | 0.05 |
| D018352 | Coronavirus Infections NIH | 0.05 |
| D012127 | Respiratory Distress Syndrome, Newborn NIH | 0.05 |
| D012128 | Respiratory Distress Syndrome, Adult NIH | 0.04 |
| D016638 | Critical Illness NIH | 0.04 |
| D011014 | Pneumonia NIH | 0.03 |
| D013577 | Syndrome NIH | 0.03 |
| D055371 | Acute Lung Injury NIH | 0.02 |
Correlated HPO Terms (7)
| Name (Synonyms) | Correlation | |
|---|---|---|
| HP:0001638 | Cardiomyopathy HPO | 0.29 |
| HP:0001402 | Hepatocellular carcinoma HPO | 0.25 |
| HP:0030358 | Non-small cell lung carcinoma HPO | 0.25 |
| HP:0030731 | Carcinoma HPO | 0.22 |
| HP:0100615 | Ovarian neoplasm HPO | 0.18 |
| HP:0001626 | Abnormality of the cardiovascular system HPO | 0.05 |
| HP:0002090 | Pneumonia HPO | 0.03 |
There are 16 clinical trials
Clinical Trials
1 Anti-MERS-COV Convalescent Plasma Therapy
Since the first report of the Middle East Respiratory Syndrome Corona virus (MERS- CoV) in September 2012, more than 800 cases have been reported to the World Health Organization (WHO) with substantial mortality.
NCT02190799 Respiratory Distress Syndrome ( Respiratory Distress Syndrome (& Respiratory Distress Syndrome (& [Hyaline Membrane Disease Respiratory Distress Syndrome (& [Hyaline Membrane Disease] Respiratory Distress Syndrome (& [Hyaline Membrane Disease]) Biological: Convalescent plasma MeSH:Respiratory Distress Syndrome, Newborn Respiratory Distress Syndrome, Adult Hyaline Membrane Disease
Primary Outcomes
Description: Hospital mortality will be death in the ICU during the same hospital admission
Measure: Hospital mortality Time: Death in the Hospital (ICU or ward) before or at 6 months after enrollmentSecondary Outcomes
Description: Death in the ICU during the same hospital admission.
Measure: ICU mortality Time: Death in the ICU at or after 90 days of enrollmentDescription: Number of calendar days between admission and final discharge from ICU.
Measure: ICU Length of Stay Time: Number of days in ICU with an average expected duration of 10 days.Description: Number of calendar days between start and final liberation from mechanical ventilation.
Measure: Duration of Mechanical Ventilation Time: Number of days of mechanical ventilation with an expected average duration of 8 daysDescription: viral clearance from all sampled sites by day 3 after administration of CP
Measure: Viral load in tracheal aspirate Time: Serial levels in the first 28 days of enrollmentDescription: Epidermal Growth Factor (EGF), Eotaxin, Granulocyte colony-stimulating factor (G-CSF), Granulocyte-Macrophage Colony-Stimulating Factor (GM-CSF), Interferon(IFN)-γ, IFN-a2, Interleukin (IL)-10, IL-12(p40), IL-12(p70), IL-13, IL-15, IL-17, IL-1ra, IL-1a, IL-1β, IL-2, IL-3, IL-4, IL-5, IL-6, IL-7, IL-8, Interferon gamma-induced protein (IP)-10, Monocyte Chemotactic Protein (MCP)-1, Macrophage Inflammatory Protein (MIP)-1a, MIP-1β, Tumor Necrosis Factor-α (TNF-a), TNF-β, Vascular Endothelial Growth Factor (VEGF)
Measure: Inflammatory markers, Time: Serial levels in the first 28 days of enrollmentDescription: anti-MERS-CoV antibody level before and after administration of CP.
Measure: Anti-MERS-CoV antibodies Time: Serial levels in the first 28 days of enrollmentOther Outcomes
Description: X ray changes at day 0, 1, 3, 7, 14, 21 and 28
Measure: Chest X ray Time: Serial changes in the X ray till day 282 Randomized, Embedded, Multifactorial Adaptive Platform Trial for Community- Acquired Pneumonia
REMAP-CAP is a randomised, embedded, multifactorial, adaptive platform trial for community-acquired pneumonia. The purpose of this study is to evaluate the effect of a range of interventions to improve outcome of patients admitted to intensive care with community-acquired pneumonia. In addition, REMAP-CAP provides and adaptive research platform for evaluation of multiple treatment modalities in the event of a respiratory pandemic resulting in critical illness. REMAP-COVID is a sub-platform of REMAP-CAP that evaluates treatments specific to COVID-19.
NCT02735707 Community-acquired Pneumonia, Influenza, COVID-19 Drug: Fixed-duration Hydrocortisone Drug: Shock-dependent hydrocortisone Drug: Ceftriaxone Drug: Moxifloxacin or Levofloxacin Drug: Piperacillin-tazobactam Drug: Ceftaroline Drug: Amoxicillin-clavulanate Drug: Macrolide administered for 3-5 days Drug: Macrolide administered for up to 14 days Drug: Five-days oseltamivir Drug: Ten-days oseltamivir Drug: Lopinavir/ritonavir Drug: Hydroxychloroquine Drug: Hydroxychloroquine + lopinavir/ritonavir Drug: Interferon-β1a Drug: Anakinra Drug: Fixed-duration higher dose Hydrocortisone Drug: Tocilizumab Drug: Sarilumab Drug: Vitamin C Drug: Therapeutic anticoagulation Drug: Simvastatin Drug: Convalescent plasma Other: Protocolised mechanical ventilation strategy MeSH:Pneumonia
HPO:Pneumonia
Primary Outcomes
Measure: All-cause mortality Time: Day 90
Description: Primary end-point for patients with suspected or proven COVID-19 pandemic infection
Measure: Days alive and not receiving organ support in ICU Time: Day 21
Secondary Outcomes
Measure: ICU Mortality Time: Day 90
Measure: ICU length of stay Time: Day 90
Measure: Hospital length of stay Time: Day 90
Measure: Ventilator free days Time: Day 28
Measure: Organ failure free days Time: Day 28
Measure: All-cause mortality Time: 6 months
Description: EQ5D-5L and WHODAS 2.0 (not completed in all regions)
Measure: Health-related Quality of life assessment Time: 6 months
Measure: Proportion of intubated patients who receive a tracheostomy Time: Day 28
Description: Characterised as home, rehabilitation hospital, nursing home or long-term care facility, or another acute hospital
Measure: Destination at time of hospital discharge Time: Free text Day 90
Measure: Readmission to the index ICU during the index hospitalization Time: Day 90
Measure: World Health Organisation 8-point ordinal scale outcome Time: Hospital discharge
Other Outcomes
Description: Antibiotic Domain specific outcome
Measure: Occurrence of multi-resistant organism colonisation/infection Time: Day 90, censored at hospital discharge
Description: Antibiotic Domain specific outcome
Measure: Occurrence clostridium difficile Time: Day 90, censored at hospital discharge
Description: Macrolide Duration domain specific outcome, and COVID-19 Antiviral Domain specific outcome.
Measure: Occurrence of serious ventricular arrhythmia (including ventricular fibrillation) or sudden unexpected death Time: Day 90, censored at hospital discharge
Description: Antiviral Domain specific outcome. Only required at selected sites.
Measure: Change from baseline influenza virus levels in upper and lower respiratory tract specimens Time: Day 3, up to Day 7
Description: COVID-19 Antiviral Domain and COVID-19 Immune Modulation Domain specific endpoint
Measure: Serial detection of SARS-CoV-2 in upper or lower respiratory tract specimens (using only specimens collected for routine clinical testing) Time: Day 90, censored at hospital discharge
3 Convalescent Plasma Therapy From Recovered Covid-19 Patients as Therapy for Hospitalized Patients With Covid-19
Primary Outcomes
Measure: All-cause mortality Time: Day 90Description: Primary end-point for patients with suspected or proven COVID-19 pandemic infection
Measure: Days alive and not receiving organ support in ICU Time: Day 21Secondary Outcomes
Measure: ICU Mortality Time: Day 90Measure: ICU length of stay Time: Day 90
Measure: Hospital length of stay Time: Day 90
Measure: Ventilator free days Time: Day 28
Measure: Organ failure free days Time: Day 28
Measure: All-cause mortality Time: 6 months
Description: EQ5D-5L and WHODAS 2.0 (not completed in all regions)
Measure: Health-related Quality of life assessment Time: 6 monthsMeasure: Proportion of intubated patients who receive a tracheostomy Time: Day 28
Description: Characterised as home, rehabilitation hospital, nursing home or long-term care facility, or another acute hospital
Measure: Destination at time of hospital discharge Time: Free text Day 90Measure: Readmission to the index ICU during the index hospitalization Time: Day 90
Measure: World Health Organisation 8-point ordinal scale outcome Time: Hospital discharge
Other Outcomes
Description: Antibiotic Domain specific outcome
Measure: Occurrence of multi-resistant organism colonisation/infection Time: Day 90, censored at hospital dischargeDescription: Antibiotic Domain specific outcome
Measure: Occurrence clostridium difficile Time: Day 90, censored at hospital dischargeDescription: Macrolide Duration domain specific outcome, and COVID-19 Antiviral Domain specific outcome.
Measure: Occurrence of serious ventricular arrhythmia (including ventricular fibrillation) or sudden unexpected death Time: Day 90, censored at hospital dischargeDescription: Antiviral Domain specific outcome. Only required at selected sites.
Measure: Change from baseline influenza virus levels in upper and lower respiratory tract specimens Time: Day 3, up to Day 7Description: COVID-19 Antiviral Domain and COVID-19 Immune Modulation Domain specific endpoint
Measure: Serial detection of SARS-CoV-2 in upper or lower respiratory tract specimens (using only specimens collected for routine clinical testing) Time: Day 90, censored at hospital dischargePassive immunization with immunoglobulins is occasionally used as therapy for the treatment of viral infectious diseases. Immunoglobulins are used for the treatment of CMV disease, and is effective as prophylaxis when given soon after exposure to varicella zoster virus, rabies, and hepatitis B virus. Neutralizing antibodies against MERS, SARS-CoV-1 and SARS-CoV-2 have been shown to be present in patients previously infected with MERS, SARS-CoV-1 and SARS-CoV-2 respectively. During the 2003 SARS outbreak in Hong-Kong,a non-randomized study in hospitalized SARS patients showed that treatment with convalescent plasma (convP) from SARS-recovered donors significantly increased the day 22 discharge rate and decreased mortality. A study in non-human primates showed that rhesus macaques could not be re-infected with SARS-CoV-2 after primary infection. With no proven effective therapy against COVID, this study will evaluate the safety and efficacy of convalescent plasma from COVID-recovered donors as a treatment for hospitalized patients with symptomatic COVID-19. The study will focus on patients who tested positive for SARS-CoV-2 in the last 96 hours before inclusion Primary objectives • Decrease overall mortality in patients within COVID disease Study design: This trial is a randomized comparative trial. Patients will be randomized between the infusion of 300mL of convP with standard of care. Patient population: Patients with PCR confirmed COVID disease, age >18 years Donors will be included with a known history of COVID who have been asymptomatic for at least 14 days. Intervention: 300mL of convP Duration of treatment: ConvP will be given as a one-time infusion Duration of follow up: For the primary endpoint: until discharge or death before day 60, whichever comes first. For the secondary endpoints (with separate consent) up to 1 year. Target number of patients: 426 Target number of donors: 100 Expected duration of accrural: 36 months
NCT04342182 COVID-19 Biological: Convalescent plasma
Primary Outcomes
Description: the mortality in the 300ml convP group will be compared with the control arm
Measure: Overall mortality until discharge from the hospital or a maximum of 60 days after admission whichever comes first Time: until hospital discharge or a maximum of 60 days whichever comes firstSecondary Outcomes
Description: the hospital days in the 300ml convP group will be compared with the control arm
Measure: Impact of 300ml convP therapy on hospital days Time: until hospital discharge or a maximum of 60 days whichever comes firstDescription: A patient will be considered weaned from oxygen therapy when the patient did not receive oxygen for at least 24 hours.
Measure: Impact of 300ml convP on weaning from oxygen therapy Time: until hospital discharge or a maximum of 60 days whichever comes firstDescription: the overall mortality in hospital days in patients admitted tot the ICU within 24 hours after admission in the 300ml convP group will be compared with the patients admitted tot the ICU within 24 hours after admission in the control arm
Measure: Impact of 300ml convP on overall mortality in patients admitted to the ICU within 24 hours after admission Time: until hospital discharge or a maximum of 60 days whichever comes firstDescription: The mortality in patients with a duration of symptoms less than the median duration of symptoms in the study population will be compared with the mortality in patients with a duration of symptoms more than the median duration of symptoms in the study population
Measure: Difference in the effect of convP on mortality in patients with a duration of symptoms less or more the median duration of symptoms in the study population Time: hospital discharge or a maximum of 60 days whichever comes firstDescription: the ICU days in hospital days in patients admitted to the ICU within 24 hours after admission in the 300ml convP group will be compared with the patients admitted tot the ICU within 24 hours after admission in the control arm
Measure: Impact of 300ml convP therapy on ICU days in patients admitted to the ICU within 24 hours after admission Time: Until hospital discharge, estimated average 4 weeksDescription: airway samples will be taken on day 1 - 3 - 5 - 7 - 10 - 14 - and at discharge
Measure: Impact of plasma therapy on the decrease in SARS-CoV2 shedding from airways Time: until hospital discharge, estimated average 2 weeksDescription: Blood wil be drawn at day 1, day 7 and day 14
Measure: Impact of CTL and NK cell immunity on the likelihood of being protected from immune serum transfer Time: until hospital discharge, extimated average 2 weeksDescription: Evaluation of Severe Adverse Events and transfusion related adverse events
Measure: Safety of convP therapy Time: until hospital discharge or a maximum of 60 days whichever comes firstDescription: The WHO COVID19 disease severity scale on day 15 will be compared with the WHO COVID19 disease severity scale on day 1
Measure: Change of the 8-point WHO COVID19 disease severity scale on day 15 Time: until day 15Description: The WHO COVID19 disease severity scale on day 30 will be compared with the WHO COVID19 disease severity scale on day 1 and day 15
Measure: Change of the 8-point WHO COVID19 disease severity scale on day 30 Time: until day 30Description: The WHO COVID19 disease severity scale on day 15 will be compared with the WHO COVID19 disease severity scale on day 1 in patients with a baseline neutralizing antibody titer (PRNT50) <80.
Measure: Change of the 8-point WHO COVID19 disease severity scale on day 15 in the subgroup of patients with a baseline neutralizing antibody titer (PRNT50) <80. Time: until day 15Description: Low dose CT and lung function is done 6 weeks after discharge and if abnormal again 3 months after discharge.
Measure: Impact of plasma therapy on risk of long-term structural lung damage and lung function Time: up to 12 months after plasma transfusion4 A Randomized Open-Label Trial of CONvalenscent Plasma for Hospitalized Adults With Acute COVID-19 Respiratory Illness (CONCOR-1)
There is currently no treatment available for COVID-19, the acute respiratory illness caused by the novel SAR-CoV-2. Convalescent plasma from patients who have recovered from COVID-19 that contains antibodies to the virus is a potential therapy. On March 25th, 2020, the FDA approved the use of convalescent plasma under the emergency investigational new drug (eIND) category. Randomized trials are needed to determine the efficacy and safety of COVID-19 convalescent plasma for acute COVID-19 infection. The objective of the CONCOR-1 trial is to determine the efficacy of transfusion of COVID-19 convalescent plasma to adult patients admitted to hospital with COVID-19 infection at decreasing the frequency of in-hospital mortality in patients hospitalized for COVID-19. It is hypothesized that treating hospitalized COVID-19 patients with convalescent plasma early in their clinical course will reduce the risk of death, and that other outcomes will be improved including risk of intubation, and length of ICU and hospital stay. This pan-Canadian clinical trial has the potential to improve patient outcomes and reduce the burden on health care resources including reducing the need for ICU beds and ventilators.
NCT04348656 COVID-19 Biological: Convalescent plasma
Primary Outcomes
Description: Endpoint of the need for intubation or patient death in hospital
Measure: Intubation or death in hospital Time: Day 30Secondary Outcomes
Description: Endpoint of the need for intubation before 30 days
Measure: Need for Intubation Time: Day 30Description: Time in hours to intubation from randomization
Measure: Time to intubation Time: Day 30Description: Endpoint of the number of days off ventilator at 30 days
Measure: Ventilator-free days Time: Day 30Description: In-hospital death censored at 90 days
Measure: In-hospital death Time: 90 daysDescription: Time to in-hospital death at 90 days
Measure: Time to in-hospital death Time: Day 90Description: Death at 30 days
Measure: Death at 30 days Time: 30 daysDescription: Date of intensive care unit admission (first date and total number of days)
Measure: Length of stay in intensive care unit (ICU) Time: Day 30Description: Date of hospital admission (first date and total number of days)
Measure: Length of stay in hospital Time: Day 30Description: First date on ECMO and total number of days
Measure: Need for extracorpeal membrane oxygenation (ECMO) Time: Day 30Description: Need for renal replacement therapy
Measure: Need for renal replacement therapy Time: Day 30Description: New myocarditis
Measure: Development of myocarditis Time: Day 30Description: Transfusion-associated adverse events, Grade 3 and 4 serious adverse events, and cumulative incidence of Grade 3 and 4 adverse events and serious adverse events (using medDRA)
Measure: Adverse events and serious adverse events Time: Day 30Description: CCP transfusion-associated adverse events (AE)
Measure: CCP transfusion-associated adverse events (AE) Time: 30 days5 COPLA Study: Treatment of Severe Forms of COronavirus Infection With Convalescent PLAsma
COVID-19 disease has become a very serious global health problem. Treatments for severe forms are urgently needed to lower mortality. Any procedure that improves these forms should be considered, especially those devoid of serious side effects.There is not enough published information on the use of allogeneic convalescent plasma (ACP) in the treatment of severe forms of COVID-19. The use of ACP can be combined with other treatments and has very few adverse effects. It takes 10-14 days for SARS-CoV2-infected patients to produce virus-neutralizing antibodies: within that time they can develop serious complications and die. Injecting PAC into patients with severe forms of COVID-19 shortens the period of risk while the patient produces the antibodies.
NCT04357106 COVID-19 Biological: Convalescent plasma MeSH:Coronavirus Infections Severe Acute Respiratory Syndrome
Primary Outcomes
Description: PaO2/FiO2 relation
Measure: Lung injury Time: 7 daysDescription: Patients survival after therapy
Measure: Overall survival Time: 15-30 daysSecondary Outcomes
Description: Determine the incidence of side effects from plasma administration
Measure: Adverse reactions to plasma Time: 7 days6 Effectiveness and Safety of Convalescent Plasma Therapy on COVID-19 Patients With Acute Respiratory Distress Syndrome in Referral Hospitals in Indonesia
Corona virus disease 2019 (COVID-19) has been declared as a Pandemic by the World Health Organization (WHO). According to WHO report on March 31st 2020, globally COVID-19 have infected over 750,000 people and caused over 36,000 deaths with case fatality rate of 4.85%. In Indonesia, COVID-19 have infected 1,414 people and caused 122 deaths with case fatality rate of 8.63%. In severe cases, COVID-19 causes complications, such as acute respiratory distress syndrome (ARDS), sepsis, septic shock, and multi-organ dysfunction syndrome (MODS), where age and comorbid illnesses as a major factor to these complications. Up to this point there are several promising therapies for COVID-19 but is not yet recommended and in need of further research. The use of convalescent plasma has been approved by the US Food and Drug Administration (FDA) through the scheme of emergency investigational new drug (eIND). This method has been used as the treatment in several outbreak or plague cases over the years, such as the flu epidemic in 1918, polio, measles, mumps, SARS (severe acute respiratory syndrome), EVD (Ebola virus disease) and MERS (middle-eastern respiratory syndrome) and this treatment shows better outcome. Several case report on the use of convalescent plasma for COVID-19 patients with ARDS and mechanical ventilation has been reported and shows promising outcome. Nevertheless, larger and multicenter research need to be done to assess and evaluate the effectiveness and safety of convalescent plasma therapy on for COVID-19 patients with ARDS.
NCT04380935 COVID Acute Respiratory Distress Syndrome Biological: Convalescent plasma Drug: Standard of care MeSH:Respiratory Distress Syndrome, Newborn Respiratory Distress Syndrome, Adult Acute Lung Injury Syndrome
Primary Outcomes
Description: Proportion of all-cause mortality
Measure: All-cause mortality Time: up to 28 daysSecondary Outcomes
Description: Mean length of stay in intensive care unit
Measure: Length of stay in intensive care unit Time: up to 28 daysDescription: Mean duration of mechanical ventilation
Measure: Duration of mechanical ventilation Time: up to 28 daysDescription: Mean change from baseline using time series analysis
Measure: Body temperature (degree in Celsius) Time: Day 1, 3, 5, and 7 after administration of therapyDescription: Mean change from baseline using time series analysis
Measure: The Sequential Organ Failure Assessment (SOFA) Score Time: Day 1, 3, 5, and 7 after administration of therapyDescription: Mean change from baseline using time series analysis
Measure: PAO2/FIO2 ratio Time: Day 1, 3, 5, and 7 after administration of therapyDescription: Mean change from baseline using time series analysis
Measure: C-Reactive Protein (CRP) in mg/L Time: Day 1, 3, 5, and 7 after administration of therapyDescription: Mean change from baseline using time series analysis
Measure: D-Dimer in ng/mL Time: Day 1, 3, 5, and 7 after administration of therapyDescription: Mean change from baseline using time series analysis
Measure: Procalcitonin in ng/mL Time: Day 1, 3, 5, and 7 after administration of therapyDescription: Mean change from baseline using time series analysis
Measure: Interleukin 6 (IL-6) in pg/mL Time: Day 1, 3, 5, and 7 after administration of therapyDescription: Number of participants with allergic/ anaphylaxis transfusion reaction
Measure: Allergic/ anaphylaxis transfusion reaction Time: 24 hours post-transfusionDescription: Number of participants with Hemolytic transfusion reaction
Measure: Hemolytic transfusion reaction Time: 24 hours post-transfusionDescription: Number of participants with Transfusion Related Acute Lung Injury
Measure: Transfusion Related Acute Lung Injury Time: 24 hours post-transfusionDescription: Number of participants with Transfusion associated Circulatory Overload
Measure: Transfusion associated Circulatory Overload Time: 24 hours post-transfusion7 Randomised Evaluation of COVID-19 Therapy
RECOVERY is a randomised trial investigating whether treatment with either Lopinavir-Ritonavir, Hydroxychloroquine, Corticosteroids, Azithromycin, Convalescent plasma or Tocilizumab prevents death in patients with COVID-19.
NCT04381936 Severe Acute Respiratory Synd Severe Acute Respiratory Syndrome Drug: Lopinavir-Ritonavir Drug: Corticosteroid Drug: Hydroxychloroquine Drug: Azithromycin Biological: Convalescent plasma Drug: Tocilizumab MeSH:Severe Acute Respiratory Syndrome Coronavirus Infections
Primary Outcomes
Description: For each pairwise comparison with the 'no additional treatment' arm, the primary objective is to provide reliable estimates of the effect of study treatments on all-cause mortality.
Measure: All-cause mortality Time: Within 28 days after randomisationSecondary Outcomes
Description: To assess the effects of study treatment on number of days stay in hospital
Measure: Duration of hospital stay Time: Within 28 days and up to 6 months after the main randomisationDescription: Among patients not on mechanical ventilation at baseline, the number of patients with a composite endpoint of death or need for mechanical ventilation or ECMO.
Measure: Composite endpoint of death or need for mechanical ventilation or ECMO Time: Within 28 days and up to 6 months after the main randomisationOther Outcomes
Description: To assess the effects of study treatment on number of patients who needed ventilation and the number of days it was required
Measure: Need for (and duration of) ventilation Time: Within 28 days and up to 6 months after the main randomisationDescription: To assess the effects of study treatment on number of patients who needed renal replacement therapy
Measure: Need for renal replacement Time: Within 28 days and up to 6 months after the main randomisationDescription: To assess the effects of study treatment on number of patients who develop new major cardiac arrythmias
Measure: Development of new major cardiac arrythmias Time: Within 28 days and up to 6 months after the main randomisation8 The Use of Convalescent Plasma for Patients Hospitalized With COVID-19 Disease
Pilot study of tolerability and efficacy of transfusion of 200mL of convalescent plasma in patients with COVID-19 respiratory disease.
NCT04385199 Coronavirus Infection Coronavirus COVID Biological: Convalescent plasma MeSH:Coronavirus Infections Severe Acute Respiratory Syndrome
Primary Outcomes
Description: For intubated patients improvement in PaO2/FiO2
Measure: Improvement in respiratory disease Time: day 1 post transfusionDescription: For intubated patients improvement in PaO2/FiO2
Measure: Improvement in respiratory disease Time: day 3 post transfusionDescription: For intubated patients improvement in PaO2/FiO2
Measure: Improvement in respiratory disease Time: day 5 post transfusionDescription: For intubated patients improvement in PaO2/FiO2
Measure: Improvement in respiratory disease Time: day 7 post transfusionDescription: For intubated patients improvement in PaO2/FiO2
Measure: Improvement in respiratory disease Time: day 14 post transfusionDescription: For intubated patients improvement in PaO2/FiO2
Measure: Improvement in respiratory disease Time: day 28 post transfusionDescription: For non intubated patients time to intubation post transfusion
Measure: Improvement in respiratory disease Time: 7 daysSecondary Outcomes
Description: ICU length of stay
Measure: ICU Length of Stay Time: 28 daysDescription: Hospital length of stay
Measure: Length of Stay Time: 28 daysDescription: Duration of time on ventilator
Measure: Ventilator days Time: 28Description: Adverse transfusion events
Measure: Tolerability of convalescent plasma Time: During transfusion, 1 day post-transfusionDescription: Improvement in Chest X Ray
Measure: Radiographic improvement Time: 3 days post transfusionDescription: Improvement in Chest X Ray
Measure: Radiographic improvement Time: 28 days post transfusion9 Efficacy of Convalescent Plasma for the Treatment of Severe SARS-CoV-2 Infection: A Randomized, Open Label Clinical Trial
Convalescent plasma has been used for over 100 years in the treatment of severe acute respiratory infections of viral origin. There are not pharmacological treatments for the actual outbreak for SARS-Cov-2 and it is necessary to evaluate the efficacy of treatment options, including convalescent plasma transfusion. The hypothesis is that convalescent plasma is efficacious and safe for reducing mortality in patients with COVID-19 treated in ICU
NCT04391101 SARS-Cov-2 Drug: Convalescent plasma
Primary Outcomes
Description: Proportion of patients who die while being hospitalized
Measure: Intrahospital mortality from any cause Time: Up to 28 daysSecondary Outcomes
Description: Number of days hospitalized
Measure: Length of hospital stay Time: Up to 60 daysDescription: Number of days without ventilatory support
Measure: Free time for ventilatory support on day 60 Time: Day 60Description: Proportion of patients alive on day 60
Measure: Overall survival at day 60 since hospitalization Time: Day 60Description: Proportion of adverse events related with convalescent plasma
Measure: Cumulative incidence of adverse events: transfusion reactions (fever, flare), TRALI (transfusion-associated lung injury), TACO (transfusion-related circulatory overload), transfusion- related infections Time: Up to 28 days10 Convalescent Plasma Transfusion Therapy in Severe COVID-19 Patients- a Tolerability, Efficacy and Dose-response Phase II RCT
As of March 18, 2020, COVID-19 cases were reported in approximately 195 countries. No specific therapeutic agents or vaccines for COVID-19 are available. Several therapies, such as remdesivir and favipiravir, are under investigation, but the antiviral efficacy of these drugs is not yet known. The use of convalescent plasma (CP) was recommended as an empirical treatment during outbreaks of Ebola virus in 2014. A protocol for treatment of Middle East respiratory syndrome coronavirus (MERS-CoV) with CP was established in 2015. This approach with other viral infections such as SARS-CoV, H5N1 avian influenza, and H1N1 influenza also suggested that transfusion of CP was effective. In previous reports, most of the patients received the CP by single transfusion. In a study involving patients with pandemic influenza A(H1N1) 2009 virus infection, treatment of severe infection with CP (n = 20 patients) was associated with reduced respiratory tract viral load, serum cytokine response, and mortality. In another study involving 80 patients with SARS, the administration of CP was associated with a higher rate of hospital discharge at day 22 from symptom onset compared with patients who did not receive CP. Accordingly, these findings raise the hypothesis that use of CP transfusion could be beneficial in patients infected with SARS-CoV-2. The objective of this study is to describe the initial clinical experience with CP transfusion administered to severe COVID-19 patients. The primary endpoint of this trial would be to assess the tolerability, efficacy, and dose-response of CP in severe COVID-19 patients. The secondary endpoint would be to assess the clinical and laboratory parameters after therapy, in-hospital mortality, length of hospital stay, reduction in the proportion of deaths, length of ICU stay, requirement of ventilator and duration of ventilator support. All RT-PCR positive cases with features of severe infection will be enrolled in this study. Apheretic CP will be collected from a recovered patient (consecutive two RT-PCR samples negative) between day 22 to 35 days of recovery and those with the antibody titre above 1:320. This RCT will consist of three arms, a. standard care, b. standard care and 200 ml CP and c. standard care and 400 ml CP as a single transfusion. Twenty (20) patients will be enrolled for each arm. Randomization will be done by someone not associated with the care or assessment of the patients by means of a random number table. Allocations will be concealed in sequentially numbered, opaque, sealed envelopes. Clinical parameters [fever, cough, dyspnea, respiratory rate, PaO2/ FiO2 level, pulse, BP, the requirement of O2, and others] will be recorded before and after CP. Laboratory parameters such as complete blood count, CRP, chest X-ray, SGPT, SGOT, S. Ferritin, and serum antibody titre will be measured before and after transfusion. Allergic or serum sickness-like reactions will be noted and adjusted with outcome. Laboratory tests including RT-PCR will be done at BSMMU virology and laboratory medicine department. Apheretic plasma will be collected at the transfusion medicine department of SHNIBPS hospital, ELISA, antibody titre will be done at CMBT, and patients will be enrolled at DMC and MuMCH. All necessary screening tests will be done before transfusion. Graphpad Prism v 7.0 will be used for analysis. One way ANOVA test, a non-parametric Mann-Whitney test, and a Kruskal-Wallis test will be performed to compare the arms. For parametric outcomes, the investigators will compare the odds ratios across the pairs.
NCT04403477 Covid19 Convalescence Biological: Convalescent plasma MeSH:Convalescence
Primary Outcomes
Description: % of patients died after enrolment
Measure: Proportion of In-hospital mortality Time: 7 daysDescription: Time to death in hours after enrolment
Measure: Time to death Time: 7 daysSecondary Outcomes
Description: Temperature in degree Fahrenheit at Day 0, 1, 3, 7
Measure: Fever Time: 7 daysDescription: Respiratory rate per minute at Day 0, 1, 3, 7
Measure: Respiratory distress Time: 7 daysDescription: Saturation of oxygen in % at Day 0, 1, 3, 7
Measure: Saturation of oxygen Time: 7 daysDescription: Blood pressure in mm of Hg at Day 0, 1, 3, 7
Measure: Blood pressure Time: 7 daysDescription: Oxygen requirements in liter/min at Day 0, 1, 3, 7
Measure: Oxygen requirement Time: 7 daysDescription: CRP level in mg/litre
Measure: C-reactive Protein Time: Day 0, 3 and 7Description: Serum Ferritin level in ng/ml
Measure: Ferritin Time: Day 0, 3 and 7Description: Serum SGPT level in I/U
Measure: SGPT Time: Day 0, 3 and 7Description: Serum SGOT level in I/U
Measure: SGOT Time: Day 0, 3 and 7Description: Duration of ICU stay in days
Measure: ICU stay Time: 14 daysDescription: Requirement of ventilator support in hours
Measure: Ventilator support Time: 14 daysDescription: Duration of hospital stay in days
Measure: Hospital stay Time: 14 daysDescription: % of patients developed early transfusion reaction like fever, sweating, rash, abdominal pain, urticaria, vomiting, wheezing, chest tightness and hypotension
Measure: Proportion of Transfusion reaction Time: 24 hours11 Convalescent Plasma Therapy in Patients With COVID-19
Scientists and medical workers all around the world were running out of time to manage COVID-19. Several studies have been done to understand the disease and ultimately to find possible treatment. Based on those studies, one of the potential treatment was antibody transfer from recovered COVID-19 patients. Passive antibody transfer was a fast and easy choice. The rational use of antibody from the patient's plasma is a natural neutralizing protein to the cell-infected virus and could possibly slow the active infection down. Investigators initiate an intervention study with purposes to produce quality convalescent plasma from the recovered patients, define the safety of plasma for human use and as an alternative treatment to improve the clinical outcomes of severe COVID-19 patients. The study hypothesis is convalescent plasma is safe and could possibly improve outcome of severe (non-critical) COVID-19 patients. This research will conduct the plaque reduction neutralizing test (PRNT) of recipient blood in vitro. The plasma will be collected in the blood transfusion unit (BTU) in Gatot Soebroto hospital. The storage, testing, transfer, and transfusion of eligible convalescent plasma are the authority of Gatot Soebroto BTU. PRNT and plasma antibody titer measurement from donor plasma will be conducted at Eijkman Institute of Molecular Biology. Investigators enroll approximately 10 patients consecutively, who will be admitted at Gatot Soebroto hospital. Baseline demographic characteristics of samples are recorded. Clinical dan laboratory data will be measured before and after plasma transfusion periodically. The measured variables are pharmacological therapy (antivirus, antibiotics, steroids), invasive oxygen therapy, oxygen index, sequential organ failure assessment (SOFA) score, and laboratory parameters such as leukocyte count, blood chemical panel include liver and renal function, C-reactive protein, procalcitonin, IL-6 and immunoglobulin titer of the recipient and also chest X-ray evaluation. The potential expected risk of plasma transfusions is transfusion reaction (immunological or non-immune related) and transferred foreign pathogen. Investigator will report and treat all adverse events after plasma transfusion has been done. A severe adverse event (SAE) will also report in a special form to sponsor and data safety monitoring board (DSMB). There is theoretically antibody-dependent enhancement (ADE) mechanism from COVID-19 whom will receive plasma transfusion to progress to severe immune response. This preliminary study is supposed to provide supporting data and experience of plasma processing to a larger study in the near future.
NCT04407208 Convalescence Corona Virus Infection Plaque Biological: Convalescent plasma MeSH:Coronavirus Infections Severe Acute Respiratory Syndrome Convalescence
Primary Outcomes
Description: PNRT50
Measure: Plaque reduction neutralization test (PNRT) Time: day 7 after first transfusionDescription: Change of D-dimer compared between pre and post transfusion
Measure: D-dimer Time: day 1,4,7,14 after first transfusionDescription: Change of CRP compared between pre and post transfusion
Measure: C-Reactive Protein (CRP) Time: day 1,4,7,14 after first transfusionDescription: Change of INR compared between pre and post transfusion
Measure: International Normalized Ratio (INR) Time: day 1,4,7,14 after first transfusionDescription: Change of OI compared between pre and post transfusion
Measure: Oxygenation Index Time: day 1,4,7,14 after first transfusionDescription: Change of CXR with CXR covid score compared between pre and post transfusion
Measure: Chest X-ray Time: day 1,4,7,28 after first transfusionSecondary Outcomes
Description: every adverse event that cause patient to die, prolonged hospitalization or worsening clinical stage of illness
Measure: severe adverse event Time: from day 0 to 14 days after plasma transfusion12 CONCOR-1: A Randomized Open-Label Trial of CONvalescent Plasma for Hospitalized Adults With Acute COVID-19 Respiratory Illness
There is currently no treatment available for COVID-19, the acute respiratory illness caused by the novel SAR-CoV-2. Convalescent plasma from patients who have recovered from COVID-19 that contains antibodies to the virus is a potential therapy. On March 25th, 2020, the FDA approved the use of convalescent plasma under the emergency investigational new drug (eIND) category. Randomized trials are needed to determine the efficacy and safety of COVID-19 convalescent plasma for acute COVID-19 infection. The objective of the CONCOR-1 trial is to determine the efficacy of transfusion of COVID-19 convalescent plasma to adult patients admitted to hospital with COVID-19 infection at decreasing the frequency of in-hospital mortality in patients hospitalized for COVID-19. It is hypothesized that treating hospitalized COVID-19 patients with convalescent plasma early in their clinical course will reduce the risk of death, and that other outcomes will be improved including risk of intubation, and length of ICU and hospital stay. WCM is a U.S. sub-site to this pan-Canadian clinical trial (NCT04348656) which has the potential to improve patient outcomes and reduce the burden on health care resources including reducing the need for ICU beds and ventilators.
NCT04418518 COVID-19 Biological: Convalescent plasma
Primary Outcomes
Description: Endpoint of the need for intubation or patient death in hospital
Measure: Intubation or death in hospital Time: Day 30Secondary Outcomes
Description: Endpoint of the need for intubation before 30 days
Measure: Need for Intubation Time: Day 30Description: Time in hours to intubation from randomization
Measure: Time to intubation Time: Day 30Description: Endpoint of the number of days off ventilator at 30 days
Measure: Ventilator-free days Time: Day 30Description: In-hospital death censored at 90 days
Measure: In-hospital death Time: 90 daysDescription: Time to in-hospital death at 90 days
Measure: Time to in-hospital death Time: Day 90Description: Death at 30 days
Measure: Death at 30 days Time: 30 daysDescription: Date of intensive care unit admission (first date and total number of days)
Measure: Length of stay in intensive care unit (ICU) Time: Day 30Description: Date of hospital admission (first date and total number of days)
Measure: Length of stay in hospital Time: Day 30Description: First date on ECMO and total number of days
Measure: Need for extracorpeal membrane oxygenation (ECMO) Time: Day 30Description: Need for renal replacement therapy
Measure: Need for renal replacement therapy Time: Day 30Description: New myocarditis
Measure: Development of myocarditis Time: Day 30Description: Transfusion-associated adverse events, Grade 3 and 4 serious adverse events, and cumulative incidence of Grade 3 and 4 adverse events and serious adverse events (using medDRA)
Measure: Adverse events and serious adverse events Time: Day 30Description: CCP transfusion-associated adverse events (AE)
Measure: CCP transfusion-associated adverse events (AE) Time: 30 days13 The Therapeutic Potential of Convalescent Plasma Therapy on Treating Critically-ill COVID-19 Patients Residing in Respiratory Care Units in Hospitals in Baghdad, Iraq
Out of 49 early-stage critically-ill COVID-19 patients, 21 patients are the experimental group who take convalescent plasma compared to 28 patients receive only conventional therapy without taking Convalescent plasma. Recovery or death, length of stay in hospital, and improvement in the clinical course of the disease are monitored in relation to monitoring through severe acute respiratory syndrome Coronavirus 2 (SARS-CoV-2) RNA detection via poly chain reaction (PCR), and SARS-CoV-2 immunoglobulin G (IgG) and immunoglobulin M (IgM) serological monitoring.
NCT04441424 IMMUNOTHERAPY Biological: Convalescent plasma Drug: Hydroxychloroquin with Azithromycin MeSH:Critical Illness
Primary Outcomes
Description: evaluate the role of convalescent plasma in saving life of treated patients by measuring the final outcome whether treated patients survived or died
Measure: Death versus survival of treated patients Time: Up to 8 weeksSecondary Outcomes
Description: this outcome is about measuring the length of stay (in days) of treated patients with convalescent plasma versus tose who were treated with conventional therapies
Measure: The length of stay in hospitals Time: Up to 8 weeks14 Infusion of Convalescent Plasma for the Treatment of Patients Infected With Severe Acute Respiratory Syndrome-Coronavirus-2 (COVID-19): A Double-blinded, Placebo-controlled, Proof-of-concept Study
Patients who are ill with COVID-19 may benefit from receiving convalescent plasma infusions containing antibodies from donors who have recovered from the disease and are proven to no longer be infected. Given the current public health emergency due to COVID-19, the FDA has recently fast-tracked the use of convalescent plasma. The purpose for this study is to assess if convalescent plasma collected from donors previously infected with Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2), the virus that causes COVID-19, can provide clinical benefit to those acutely ill with the virus and to evaluate if such treatment is safe. There will be two arms in the interventional study, where subjects will either be treated with convalescent plasma or fresh frozen plasma in a randomized and blinded manner. As an additional comparison, the clinical course of subjects enrolled during the period of the study who do not receive an alternative treatment for COVID-19 will be assessed.
NCT04442191 COVID-19 Biological: Convalescent plasma Biological: Placebo
Primary Outcomes
Description: The primary endpoint will be clinical response at 8 days, defined as no need for oxygen supplementation for the previous 24 hours.
Measure: Oxygen supplementation Time: 8 daysSecondary Outcomes
Description: Mortality rate during the 28 days of follow-up and during the subjects' initial hospital stays
Measure: 28-day and in-hospital mortality rate Time: 28 daysDescription: Transfer to an ICU bed during the 28 days following study enrollment
Measure: Number of participants transferred to the Intensive Care Unit (ICU) Time: 28 daysDescription: Intubation within the 28 days following study enrollment
Measure: Number of participants intubated Time: 28 daysDescription: Number of days admitted to the hospital during the 28-day follow-up period
Measure: Length of hospital stay in days Time: 28 daysDescription: Type of respiratory support required during the 28-day follow-up period: intubation, high-flow oxygen by nasal canula, nasal canula
Measure: Type of respiratory support Time: 28 daysDescription: Change in CRP following treatment
Measure: C-reactive Protein (CRP) Time: 28 daysDescription: Change in lymphocyte count following treatment
Measure: Lymphocyte count Time: 28 daysDescription: Number of days respiratory support is required
Measure: Length or respiratory support required, in days Time: 28 daysDescription: Change in LDH following treatment
Measure: Lactate dehydrogenase (LDH) Time: 28 daysDescription: Change in Ferritin level following treatment
Measure: Ferritin Time: 28 daysDescription: Change in D-Dimer level following treatment
Measure: D-Dimer Time: 28 daysDescription: Change in WBC count following treatment
Measure: White Blood Cell (WBC) Count Time: 28 daysOther Outcomes
Description: Severe transfusion reaction will be defined as having any of the following occur within 6 hours of the infusion of blood product and not attributable to the underlying disease: 1) an increase of 2 L/minutes or more in supplemental oxygen requirement compared to the baseline requirement before transfusion, 2) oxygen saturations <93% despite oxygen via nasal canula, or 3) need for transfer to the ICU.
Measure: Safety endpoint: Severe transfusion reaction Time: 6 hours following transfusionDescription: Cumulative incidence of adverse events during the study period: transfusion reaction (fever, rash), transfusion related acute lung injury (TRALI), transfusion associated circulatory overload (TACO), transfusion related infection.
Measure: Safety endpoint two: adverse events Time: 24 hours following transfusion15 Pilot Clinical, Statistical and Epidemiological Study on Efficacy and Safety of Convalescent Plasma for the Management of Patients With COVID-19
The health contingency established against the Severe Acute Respiratory Syndrome associated type 2 Coronavirus (SARS-CoV-2) has promoted a race against the clock for the search on treatment against the disease related with coronavirus (COVID-19). There are no current approved therapeutic options against the virus, although there is a rush for the development of drugs, vaccines and even the passive immunization through plasma from convalescent patients. This passive immunization is made with the administration of antibodies from patients that went through the infectious state of the disease and progress to clinical remission. SARS-CoV-2, and its predecessor SARS-CoV-1, have great similarities between their genes and proteins; tis allow to hypothesize that the antibodies developed against SARS-CoV1 can recognize the antigens of SARS-CoV-2. In this manner, the transfusion of convalescent plasma to patients with the infection brings the probability on eliminating the infection, in this case SARS-CoV-2. There are evidence of this phenomenon observed in previous pandemics caused by SARS-CoV-1, Influenza AH1N1 and Ebola virus. The objective of the study is to develop a therapeutic strategy based on the administration of plasma from patients with COVID-19 with clinical remission to patients that are coursing with the infection. The expected results hopes to establish an effective treatment and satisfactory recovery of patients with COVID-19. Also, we expect to describe the respective antibodies related against the SARS-CoV-2 infection.
NCT04452812 COVID-19 Pneumonia Convalescent Plasma Biological: Convalescent plasma MeSH:Pneumonia
HPO:Pneumonia
Primary Outcomes
Description: Any cause mortality during the first 30 days of treatment
Measure: All-cause mortality Time: 30 days
Description: Side effects associated with the administration of convalescent plasma
Measure: Side effects Time: 30 days
Secondary Outcomes
Description: Time to discharge from the ICU
Measure: Length of stay in Intensive Care Unit (ICU) Time: 14 days
Description: Time for discharge from hospital
Measure: Length of stay in hospitalization Time: 21 days
Description: Number of days with ventilatory support
Measure: Days of mechanical ventilation Time: 14 days
Description: change in D-dimer (micrograms/L)
Measure: Inflammatory biomarkers (d-dimer) Time: 21 days
Description: change in C-reactive protein (milligrams/dL)
Measure: Inflammatory biomarkers (c-reactive protein) Time: 21 days
Description: Change in LDH (UI/L)
Measure: Inflammatory biomarkers (lactate dehydrogenase) Time: 21 days
Description: Change in ferritin (nanograms/mL)
Measure: Inflammatory biomarkers (ferritin) Time: 21 days
16 Treatment of Critically Ill Patients With Covid-19 With Convalescent Plasma
Primary Outcomes
Description: Any cause mortality during the first 30 days of treatment
Measure: All-cause mortality Time: 30 daysDescription: Side effects associated with the administration of convalescent plasma
Measure: Side effects Time: 30 daysSecondary Outcomes
Description: Time to discharge from the ICU
Measure: Length of stay in Intensive Care Unit (ICU) Time: 14 daysDescription: Time for discharge from hospital
Measure: Length of stay in hospitalization Time: 21 daysDescription: Number of days with ventilatory support
Measure: Days of mechanical ventilation Time: 14 daysDescription: change in D-dimer (micrograms/L)
Measure: Inflammatory biomarkers (d-dimer) Time: 21 daysDescription: change in C-reactive protein (milligrams/dL)
Measure: Inflammatory biomarkers (c-reactive protein) Time: 21 daysDescription: Change in LDH (UI/L)
Measure: Inflammatory biomarkers (lactate dehydrogenase) Time: 21 daysDescription: Change in ferritin (nanograms/mL)
Measure: Inflammatory biomarkers (ferritin) Time: 21 daysThis study aims to collect convalescent plasma and use it as experimental treatment in critically ill Covid-19 patients in order to reduce mortality and length of stay in intensive care unit.
NCT04468009 SARS-Associated Coronavirus Covid19 SARS-CoV Infection Biological: Convalescent plasma MeSH:Coronavirus Infections Severe Acute Respiratory Syndrome
Primary Outcomes
Description: Mortality at 30 days of Intensive Care Unit (ICU) admission
Measure: Mortality at ICU at 30 days Time: Mortality at 30 daysDescription: Mortality at 90 days of ICU admission
Measure: Mortality at ICU at 90 days Time: Mortality at 90 daysSecondary Outcomes
Description: Sequential Organ Failure Assessment (SOFA) of study days 1, 3, 5, 7, 14 and 28
Measure: SOFA score of study days 1, 3, 5, 7, 14 and 28 Time: Study days 1, 3, 5, 7, 14 and 28Description: Duration (number of days) of supportive therapy (oxygen and ventilation, dialysis, vasopressors) after enrollment
Measure: Need for supportive therapy after enrollment Time: Duration of supportive therapy through study completion, an average of 3 monthsDescription: Duration (number of days) of stay in ICU between ICU admission and ICU final discharge
Measure: Lenght of stay in ICU Time: Duration of stay in ICU through study completion, an average of 3 monthsDescription: Duration (number of days) of mechanical ventilation between beginning and final liberation from mechanical ventilation
Measure: Lenght of mechanical ventilation Time: Duration of mechanical ventilation through study completion, an average of 3 monthsDescription: Duration (number of days) of hospitalization between hospital admission and final hospital discharge
Measure: Lenght of hospitalization Time: Duration of hospitalization through study completion, an average of 3 monthsOther Outcomes
Description: Duration (number of days) of hospitalization after ICU discharge
Measure: Lenght of hospitalization after ICU discharge Time: Duration (number of days) of hospitalization through study completion, an average of 3 monthsDescription: Number of days without ventilation after enrollment
Measure: Days without ventilation after enrollment Time: Days without ventilation through study completion, an average of 3 monthsDescription: Number of days without vasopressors after enrollment
Measure: Days without vasopressors after enrollment Time: Days without vasopressors through study completion, an average of 3 monthsDescription: Changes in Chest X-ray (unilateral, bilateral, unique, multiple, pleural effusion) after enrollment
Measure: Changes in Chest X-ray Time: Changes in Chest X-ray through study completion, an average of 3 months