Hemorrhagic Fever, Ebola Clinical Trial
Official title:
Emergency Evaluation of Convalescent Plasma for Ebola Viral Disease (EVD) in Guinea
This is an emergency, phase 2/3, open-label, non-randomized, clinical trial that will
evaluate Convalescent Plasma (CP) added to standardized supportive care (SC) in patients with
confirmed Ebola Virus Disease (EVD). No patient will be refused CP when compatible products
are available and all efforts will be made to maximize CP availability during the study. EVD
patients recruited during the period before CP becomes available or for whom no compatible CP
is available will be given SC and will be followed for study outcomes. Data from these SC
patients will be the used as comparator in the analysis of the study. The primary objective
of the study is to assess if CP + SC improves the 14 day survival of patients, compared to SC
alone.
The Investigators aim to enroll a total number of 130 - 200 patients who will be treated
treated with CP assuming equal numbers of patients treated with SC alone. If there would be
insufficient patients treated with SC, patients treated at the research site prior to study
start may be included in the comparison group.
Patients will be recruited in the Ebola Treatment centre managed by Medecins Sans Frontieres
(MSF) in Conakry, Guinea. All patients and/or relatives presenting at the centre will be
informed about the study, and will be invited to provide consent at the time of admission
inside the treatment centre. Only patients for whom ebola infection is confirmed with
polymerase chain reaction (PCR) will be enrolled in the study. After inclusion, eligibility
to the intervention will be reassessed on regular intervals. If the eligibility criteria are
not met by 48 hours after inclusion, only SC will be continued.
In line with the guidance of the World Health Organization (WHO), two units of CP will be
given. EVD patients will be transfused with ABO-compatible CP using standard procedures.
Details on the modalities of transfusion can be found in the WHO guidance document and the
MSF guidelines on blood transfusion. All patients will be under close observation for
transfusion-related adverse reactions during and up to 4 hours after transfusion. 24 hours
after the start of transfusion, a blood sample will be collected for viral load assessment.
All other aspects of patient management will be according to MSF clinical guidelines. The
decision to discharge a patient should be taken on clinical grounds, but can be supported by
the laboratory results. After discharge, the patient will be followed up by the study team
until day 30.
West-Africa is being ravaged by the worst outbreak of Ebola Viral Disease (EVD) ever
witnessed. Nine months after its onset, the outbreak has spiraled and currently appears to be
out of control. One of the key factors contributing to the high mortality is the lack of any
proven effective EVD specific treatment. The identification of effective therapies is a
medical and public health priority. Convalescent whole blood (CWB) and convalescent plasma
(CP) have been prioritized by the World Health Organization (WHO) to be evaluated within a
short time span, so that widespread use for therapy could be implemented rapidly if proven
effective. Both CWB and CP contain EBV antibodies and either could potentially be of value as
EVD therapy, however their efficacy in Ebola must still be demonstrated. .
This is an emergency, phase 2/3, open-label, non-randomized, clinical trial that will
evaluate CP added to standardized supportive care (SC) in patients with confirmed EVD. No
patient will be refused CP when compatible products are available and all efforts will be
made to maximize CP availability during the study. EVD patients recruited during the period
before CP becomes available or for whom no compatible CP is available will be given SC and
will be followed for study outcomes. Data from these SC patients will be the used as
comparator in the analysis of the study.
The primary objective of the study is to assess if CP + SC improves the 14 day survival of
patients, compared to SC alone. Secondary objectives are;
- to assess 30 day survival on CP + SC
- to assess the relationship between EV antibody levels in donated CP and survival in
patients receiving CP
- to assess the relationship between EV antibody levels in donated CP and changes in
levels of viral RNA in the blood of patients receiving CP
- to assess the occurrence of serious adverse reactions (SARs) related to CP transfusion
in Ebola patients
- to assess the occurrence of safety risks related to CP transfusion in health workers
administering the treatments
- to determine risk factors for mortality despite administration of CP (for identification
of patients most likely to benefit)
The Investigators aim to enroll a total number of 130 - 200 patients treated with CP assuming
equal numbers of patients treated with SC alone. The number of patients treated with SC will
be determined by the time interval for CP to become available for treatment and the
availability of CP throughout the study. If there would be insufficient patients treated with
SC, patients treated at the research site prior to study start may be included in the
comparison group.
Patients will be recruited in the Ebola Treatment centre managed by Medecins Sans Frontieres
(MSF) in Conakry. All patients and/or relatives presenting at the centre will be informed
about the study, and will be invited to provide consent at the time of admission inside the
treatment centre. Only patients for whom ebola infection is confirmed via polymerase chain
reaction (PCR) will be enrolled in the study. After inclusion, eligibility to the
intervention will be assessed at the time of enrollment (when the patient is moved to the
area for patients with confirmed Ebola) and will be reassessed on regular intervals as long
as the patient did not receive plasma transfusion. The re-assessment of eligibility to
receive CP happens at 8h and at 12h, and is repeated until 48 hours after inclusion. If the
eligibility criteria are not met by 48 hours after inclusion, only SC will be continued.
A patient is not eligible to receive CP if they meet one of the following criteria:
- History of allergic reaction to blood or plasma products (as judged by the investigator
or treating physician); (this first criterion is definite and will not be re-assessed)
- Medical conditions in which receipt of additional fluid related to the transfusion
(250-500 ml or in the case of children 10 ml/kg) may be detrimental to the patient (e.g.
decompensated congestive heart failure or renal failure).
- Patients in shock unresponsive to fluid challenge
- Patients in shock with signs of multi-organ failure, defined as oliguria/anuria AND
impaired consciousness AND/OR jaundice
- Condition of patient where the procedure of plasma administration carries a risk for the
staff
In line with the WHO guidance, two units of CP will be given. EVD patients will be transfused
with ABO-compatible CP using standard procedures. Details on the modalities of transfusion
can be found in the WHO guidance document and the MSF guidelines on blood transfusion. All
patients will be under close observation for transfusion-related adverse reactions during and
up to 4 hours after transfusion. 24 hours after the start of transfusion, a blood sample will
be collected for viral load assessment. All other aspects of patient management will be
according to MSF clinical guidelines.
The decision to discharge a patient should be taken on clinical grounds, but can be supported
by the laboratory results. After discharge, the patient will be followed up by the study team
until day 30.
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