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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02572817
Other study ID # IRC-005
Secondary ID
Status Completed
Phase Phase 3
First received
Last updated
Start date November 2015
Est. completion date May 18, 2018

Study information

Verified date June 2019
Source National Institute of Allergy and Infectious Diseases (NIAID)
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This study assessed the efficacy and safety of anti-influenza immune plasma, as an addition to standard of care antivirals, in participants hospitalized with severe influenza A infection.


Description:

Despite antivirals and vaccines, influenza is responsible for thousands of hospitalizations and deaths each year worldwide. Because of this, additional treatments for influenza are needed. One potential treatment may be the use of high-titer anti-influenza immune plasma. The purpose of this study is to evaluate the efficacy and safety of treatment with high-titer versus low-titer anti-influenza immune plasma, in addition to standard care, in participants hospitalized with severe influenza A infection.

This study enrolled people aged 2 weeks or older who are hospitalized with severe influenza A infection. Participants were randomly assigned to receive either high-titer anti-influenza plasma or low-titer (control) anti-influenza plasma on Day 0. In addition, all participants received standard care antivirals. Participants were assessed on Day 0 (baseline) and on Days 1, 2, 3, 7, 14, and 28. For participants who were not hospitalized on Days 2, 14, and 28, researchers could contact participants by telephone. Study procedures included clinical assessments, blood collection, and oropharyngeal swabs.


Other known NCT identifiers
  • NCT02610478

Recruitment information / eligibility

Status Completed
Enrollment 138
Est. completion date May 18, 2018
Est. primary completion date April 26, 2018
Accepts healthy volunteers No
Gender All
Age group N/A and older
Eligibility Inclusion Criteria for Enrollment (Screening):

- Subjects must be aged 2 weeks or older.

- Hospitalization due to signs and symptoms of influenza.

* Note: The decision for hospitalization will be made by the treating clinician. To be considered eligible, the hospitalization may either be an initial hospitalization, or a prolongation of a hospitalization due to a respiratory illness that was found to be from influenza. Influenza could be a component of a larger respiratory syndrome (i.e. COPD exacerbation thought to be triggered by influenza). However, respiratory syndromes that are not likely due to the virus should not be included (i.e. a subject that had mild influenza then developed pulmonary embolism and respiratory distress from the embolism).

- Study plasma available on-site or available within 24 hours after randomization.

- Not previously screened nor randomized in this study.

- Willingness to have blood and respiratory samples obtained and stored.

- Willingness to return for all required study visits and participate in study follow up.

Inclusion Criteria for Randomization:

- Locally determined positive test for influenza A (by polymerase chain reaction [PCR], other nucleic acid testing, or by rapid Ag) from a specimen obtained less than or equal to 48 hours prior to randomization.

- Onset of illness less than or equal to 6 days before randomization, defined as when the subject first experienced at least one respiratory symptom or fever.

- Note: For subjects with chronic respiratory symptoms (chronic cough, or COPD with baseline dyspnea), the onset of symptoms is defined as the point when the symptoms changed during this illness). Hospitalized due to influenza, with anticipated hospitalization for more than 24 hours after randomization. Criteria for hospitalization will be up to the individual treating clinician.

- National Early Warning (NEW) or Pediatric Early Warning (PEW) score greater than or equal to 3 within 12 hours prior to randomization.

- ABO-compatible plasma available on-site or available within 24 hours after randomization.

Exclusion Criteria for Randomization:

- Strong clinical evidence in the judgment of the site investigator that the etiology of illness is primarily bacterial super-infection in origin. Co-infection would be allowed, as there may be benefit to resolving influenza illness faster. Super-infection, where influenza illness occurred and is resolving, and new bacterial illness causing deterioration should be excluded (e.g., if the subject's respiratory infection is thought unlikely to benefit from additional antiviral therapy, this exclusion criteria would be met).

- Prior treatment with any anti-influenza investigational drug, anti-influenza investigational intravenous immune globulin (IVIG), or anti-influenza investigational plasma therapy within 30 days prior to screening. Other investigational drug therapies (non-influenza) and administration of plasma and/or IVIG for non-influenza reasons are allowed.

- History of allergic reaction to blood or plasma products (as judged by the site investigator).

- A pre-existing condition or use of a medication that, in the opinion of the site investigator, may place the individual at a substantially increased risk of thrombosis (e.g., cryoglobulinemia, severe refractory hypertriglyceridemia, or clinically significant monoclonal gammopathy). Prior IVIG use alone would not meet exclusion criteria, but the investigator should consider the potential for a hyper-coagulable state.

- Subjects who, in the judgment of the site investigator, will be unlikely to comply with the requirements of this protocol, including being not contactable following discharge from hospital.

- Medical conditions for which receipt of 500-600 mL (or pediatric equivalent) of intravenous fluid may be dangerous to the subject (e.g., decompensated congestive heart failure).

Study Design


Intervention

Biological:
High-titer anti-influenza plasma
Human plasma (FFP or FP24, 225-350 mL per unit or pediatric equivalent) with both an influenza A/H1N1 and A/H3N2 HAI titer of at least 1:80
Low-titer anti-influenza plasma
Human plasma (FFP or FP24, 225-350 mL per unit or pediatric equivalent) with both an influenza A/H1N1 and A/H3N2 HAI titer of 1:10 or less

Locations

Country Name City State
United States University of Michigan Ann Arbor Michigan
United States Children's Hospital Colorado Aurora Colorado
United States University of Colorado Denver Aurora Colorado
United States Johns Hopkins University Baltimore Maryland
United States University of Maryland Medical Center Baltimore Maryland
United States Boston Children's Hospital Boston Massachusetts
United States Massachusetts General Hospital Boston Massachusetts
United States Bridgeport Hospital Bridgeport Connecticut
United States University of Vermont Burlington Vermont
United States Carolinas Medical Center Charlotte North Carolina
United States Rush University Medical Center Chicago Illinois
United States Cincinnati Children's Hospital Medical Center Cincinnati Ohio
United States University of Cincinnati Cincinnati Ohio
United States UT Southwestern Medical Center Dallas Texas
United States Duke University Durham North Carolina
United States University of Florida Gainesville Florida
United States UCLA Pediatrics Infectious Diseases Los Angeles California
United States New York University/Bellevue Hospital New York New York
United States University of Oklahoma Health Sciences Center Oklahoma City Oklahoma
United States Creighton University Medical Center Omaha Nebraska
United States University of Pennsylvania Philadelphia Pennsylvania
United States University of Pittsburgh Medical Center Pittsburgh Pennsylvania
United States Mayo Clinic Campus Saint Mary's Rochester Minnesota
United States Beaumont Hospital - Royal Oak Royal Oak Michigan
United States St. Louis Children's Hospital at Washington University Saint Louis Missouri
United States Naval Medical Center San Diego (NMCSD) San Diego California
United States Madigan Army Medical Center (MAMC) Tacoma Washington
United States Beaumont Hospital, Troy Troy Michigan
United States University of Arizona Health Sciences Center Tucson Arizona
United States University of Massachusetts Medical School Worcester Massachusetts

Sponsors (1)

Lead Sponsor Collaborator
National Institute of Allergy and Infectious Diseases (NIAID)

Country where clinical trial is conducted

United States, 

References & Publications (6)

Leteurtre S, Duhamel A, Grandbastien B, Lacroix J, Leclerc F. Paediatric logistic organ dysfunction (PELOD) score. Lancet. 2006 Mar 18;367(9514):897; author reply 900-2. — View Citation

Leteurtre S, Martinot A, Duhamel A, Proulx F, Grandbastien B, Cotting J, Gottesman R, Joffe A, Pfenninger J, Hubert P, Lacroix J, Leclerc F. Validation of the paediatric logistic organ dysfunction (PELOD) score: prospective, observational, multicentre study. Lancet. 2003 Jul 19;362(9379):192-7. Erratum in: Lancet. 2006 Mar 18;367(9514):902. Lancet. 2006 Mar 18;367(9514):897; author reply 900-2. — View Citation

Parshuram CS, Bayliss A, Reimer J, Middaugh K, Blanchard N. Implementing the Bedside Paediatric Early Warning System in a community hospital: A prospective observational study. Paediatr Child Health. 2011 Mar;16(3):e18-22. — View Citation

Smith GB, Prytherch DR, Meredith P, Schmidt PE, Featherstone PI. The ability of the National Early Warning Score (NEWS) to discriminate patients at risk of early cardiac arrest, unanticipated intensive care unit admission, and death. Resuscitation. 2013 Apr;84(4):465-70. doi: 10.1016/j.resuscitation.2012.12.016. Epub 2013 Jan 4. — View Citation

Vincent JL, de Mendonça A, Cantraine F, Moreno R, Takala J, Suter PM, Sprung CL, Colardyn F, Blecher S. Use of the SOFA score to assess the incidence of organ dysfunction/failure in intensive care units: results of a multicenter, prospective study. Working group on "sepsis-related problems" of the European Society of Intensive Care Medicine. Crit Care Med. 1998 Nov;26(11):1793-800. — View Citation

Vincent JL, Moreno R, Takala J, Willatts S, De Mendonça A, Bruining H, Reinhart CK, Suter PM, Thijs LG. The SOFA (Sepsis-related Organ Failure Assessment) score to describe organ dysfunction/failure. On behalf of the Working Group on Sepsis-Related Problems of the European Society of Intensive Care Medicine. Intensive Care Med. 1996 Jul;22(7):707-10. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary Clinical Status at Day 7 The clinical status at Day 7 was based on a 6-point ordinal scale:
Death
In ICU
Non-ICU hospitalization, requiring supplemental oxygen (O2)
Non-ICU hospitalization, not requiring supplemental oxygen
Not hospitalized, but unable to resume normal activities
Not hospitalized with full resumption of normal activities A higher score corresponds to a better health outcome
Day 7
Secondary Clinical Status at Day 1 The clinical status at Day 1 was based on a 6-point ordinal scale:
Death
In ICU
Non-ICU hospitalization, requiring supplemental oxygen (O2)
Non-ICU hospitalization, not requiring supplemental oxygen
Not hospitalized, but unable to resume normal activities
Not hospitalized with full resumption of normal activities A higher score corresponds to a better health outcome
Day 1
Secondary Clinical Status at Day 2 The clinical status at Day 2 was based on a 6-point ordinal scale:
Death
In ICU
Non-ICU hospitalization, requiring supplemental oxygen (O2)
Non-ICU hospitalization, not requiring supplemental oxygen
Not hospitalized, but unable to resume normal activities
Not hospitalized with full resumption of normal activities A higher score corresponds to a better health outcome
Day 2
Secondary Clinical Status at Day 3 The clinical status at Day 3 was based on a 6-point ordinal scale:
Death
In ICU
Non-ICU hospitalization, requiring supplemental oxygen (O2)
Non-ICU hospitalization, not requiring supplemental oxygen
Not hospitalized, but unable to resume normal activities
Not hospitalized with full resumption of normal activities A higher score corresponds to a better health outcome
Day 3
Secondary Clinical Status at Day 14 The clinical status at Day 14 was based on a 6-point ordinal scale:
Death
In ICU
Non-ICU hospitalization, requiring supplemental oxygen (O2)
Non-ICU hospitalization, not requiring supplemental oxygen
Not hospitalized, but unable to resume normal activities
Not hospitalized with full resumption of normal activities A higher score corresponds to a better health outcome
Day 14
Secondary Clinical Status at Day 28 The clinical status at Day 28 was based on a 6-point ordinal scale:
Death
In ICU
Non-ICU hospitalization, requiring supplemental oxygen (O2)
Non-ICU hospitalization, not requiring supplemental oxygen
Not hospitalized, but unable to resume normal activities
Not hospitalized with full resumption of normal activities A higher score corresponds to a better health outcome
Day 28
Secondary Duration of Initial Hospitalization Duration (in days) of initial hospitalization, restricted to duration between randomization and last visit From Day 0 to Day 28
Secondary 28-day Mortality Number of deaths during study follow-up From Day 0 to Day 28
Secondary In-hospital Mortality During Initial Hospitalization Number of deaths in the hospital during initial hospitalization From Day 0 to Day 28
Secondary Composite of Mortality and Hospitalization at Day 7, Day 14, Day 28 Two categories were considered for the composite of mortality and hospitalization:
Dead or hospitalized Alive and not hospitalized
Day 7, Day 14, Day 28
Secondary Change From Baseline to Day 3 and Day 7 in National Early Warning (NEW) Score The National Early Warning (NEW) score was only measured for the adult participants.
The range of the NEW score is from 0 to 20, with lower values representing a better outcome.
Baseline is defined as the Day 0. Change was defined as the value at Day 3 or Day 7 minus the value at baseline.
Day 0, Day 3, Day 7
Secondary Change From Baseline to Day 3 and Day 7 in Pediatric Early Warning (PEW) Score The Pediatric Early Warning (PEW) score was only measured for the pediatric participants.
The range is from 0 to 26, with lower values representing a better outcome. Baseline is defined as the Day 0. Change was defined as the value at Day 3 or Day 7 minus the value at baseline.
Day 0, Day 3, Day 7
Secondary Duration of Supplemental Oxygen Duration (in days) of total supplemental oxygen use among those participants who required new or increased oxygen at randomization.
The duration is restricted to duration between randomization and last visit.
From Day 0 to Day 28 visit. The window of the Day 28 visit was 28-32 days from study entry.
Secondary Incidence of New Oxygen Use During the Study Incidence of new oxygen use during the study among those participants who did not require oxygen at randomization From Day 0 to Day 28
Secondary Duration of Intensive Care Unit (ICU) Stay Duration (in days) of ICU stay among those participants who were in ICU at randomization.
The duration is restricted to duration between randomization and last visit.
From Day 0 to Day 28
Secondary Incidence of New ICU Admission Use During the Study Incidence of new ICU admission during the study among those participants who were not in ICU at randomization From Day 0 to Day 28
Secondary Duration of Mechanical Ventilation Use Duration (in days) of mechanical ventilation use among those participants who were on mechanical ventilation at randomization.
The duration is restricted to duration between randomization and last visit.
From Day 0 to Day 28 visit. The window of the Day 28 visit was 28-32 days from study entry
Secondary Incidence of New Mechanical Ventilation Use Stay Use During the Study Incidence of new mechanical ventilation use during the study among those participants who were not on mechanical ventilation at randomization From Day 0 to Day 28
Secondary Duration of Acute Respiratory Distress Syndrome (ARDS) Duration (in days) of ARDS use among those participants with ARDS at randomization.
The duration is restricted to duration between randomization and last visit.
From Day 0 to Day 28
Secondary Incidence of New ARDS During the Study Incidence of new ARDS during the study among those participants without ARDS at randomization From Day 0 to Day 28
Secondary Duration of Extracorporeal Membrane Oxygenation (ECMO) Duration (in days) of ECMO use among those participants on ECMO at randomization.
The duration is restricted to duration between randomization and last visit.
From Day 0 to Day 28
Secondary Incidence of New ECMO Use During the Study Incidence of new ECMO use during the study among those participants not on ECMO at randomization From Day 0 to Day 28
Secondary Change From Baseline to Day 3 and Day 7 in Sequential Organ Failure Assessment (SOFA) Score The Sequential Organ Failure Assessment (SOFA) score was only measured for the adult participants.
The range is from 0 to 24, with lower values representing a better outcome. Baseline is defined as the Day 0. Change was defined as the value at Day 3 or Day 7 minus the value at baseline.
Day 0, Day 3, Day 7
Secondary Change From Baseline to Day 3 and Day 7 in Pediatric Logistic Organ Dysfunction (PELOD) Score The Pediatric Logistic Organ Dysfunction (PELOD) score was only measured for the pediatric participants.
The range is from 0 to 71, with lower values representing a better outcome. Baseline is defined as the Day 0. Change was defined as the value at Day 3 or Day 7 minus the value at baseline.
Day 0, Day 3, Day 7
Secondary Disposition After Initial Hospitalization Disposition at discharge after initial hospitalization was categorized as follows:
Death, Ongoing at 28 days, Chronic nursing facility, Rehabilitation, Home with home health care, Home without assistance.
The number of deaths at discharge after initial hospitalization do not necessarily match the overall number of deaths.
From Day 0 to Day 28
Secondary Detectable Influenza Virus at Day 3 Detectable influenza virus at Day 3 in oropharyngeal samples Day 3
Secondary Hemagglutination Inhibition Assay (HAI) Titers at Days 1, 3, 7 for A/H1N1 Hemagglutination inhibition assay (HAI) titers as measured by serial dilutions at Days 1, 3, 7 for A/H1N1. HAI for A/H1N1 was tested in all influenza seasons while the study was ongoing. Day 1, Day 3, Day 7
Secondary Hemagglutination Inhibition Assay (HAI) Titers at Days 1, 3, 7 for A/HongKong/4801/2014 H3N2 Hemagglutination inhibition assay (HAI) titers as measured by serial dilutions at Days 1, 3, 7 for A/HongKong/4801/2014 H3N2. HAI for A/HongKong/4801/2014 H3N2 was tested in all influenza seasons while the study was ongoing. Day 1, Day 3, Day 7
Secondary Number of Participants With Grade 3 and 4 Adverse Events (AEs). Number of participants with reported grade 3 and 4 adverse events (AEs) throughout the study duration. In cases where participants had multiple reports of grade 3 and 4 AEs, they were only counted once. From Day 0 to Day 28
Secondary Number of Participants With Serious Adverse Events (SAEs). Number of participants with reported serious adverse events (SAEs) throughout the study duration. From Day 0 to Day 28
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