Coronary Artery Disease Clinical Trial
Official title:
"Salvage Use" of Recombinant Activated Factor VII After Inadequate Haemostatic Response to Conventional Therapy in Complex Cardiac Surgery - a Randomised Placebo Controlled Trial
Aims and Hypotheses:
This randomised placebo controlled study will test the hypothesis that Recombinant Activated
Factor VII (rVIIa) will improve haemostasis after an inadequate response to conventional
therapy in complex cardiac surgery.
Major bleeding is still of concern in complex cardiac surgery. It has been shown to be
associated with poorer patient outcome and results in the consumption of resources (hospital
costs, manpower and blood bank reserves). This study has the potential to provide evidence
that rVIIa can reduce transfusion requirements and improve patient outcome in a problematic
aspect of complicated cardiac surgery.
The objective is to conduct a multi-centre randomised placebo controlled study that has been
designed to scientifically evaluate the treatment of post bypass coagulopathy in the
association with complex cardiac surgery. The trial design is based on clinical practice
that has evolved over 2 years at the Austin Hospital during which 38 patients have received
open label administration of rVIIa. There is currently no published RCT in this area and
there is no TGA approval for the use of rVIIa for this indication.
11. 3 Methods
Synopsis of Study:
A multicentred randomised, double blind, placebo-controlled trial evaluating the efficacy
and safety of activated recombinant factor VII (rVIIa) in complex cardiac surgery.
Study will be conducted at Austin Hospital, Alfred Hospital and Warringal Private Hospital.
The study will have two arms:
1. Those who have inadequate haemostasis after initial standardised administration of
coagulation factors and receive rVIIa. (Active arm)
2. Those who have inadequate haemostasis after initial standardised administration of
coagulation factors and receive placebo. (Placebo arm)
We anticipate from our preliminary series that 50% of enrolled subjects will achieve
haemostasis after the initial standardised dose of coagulation factors and therefore
don’t receive trial medication. Identical data will be collected and will form an
observational subgroup for analysis.
The protocol allows for open label administration of rVIIa if adequate haemostasis is
not achieved after two standardised administrations of coagulation factors and the
trial medication. This would be within 2 hours of the completion of the first
administration
Primary endpoint will be “adequate haemostasis to enable chest closure” after
administration of trial medication without the need for further intervention to improve
coagulation.
Secondary Endpoints, percentage of cases that haemostasis after first administration of
coagulation factors alone Assessment of surgical field after administration of trial
medication Time to closure of chest after administration of trial medication
Transfusion requirements in post bypass period in theatre Transfusion requirements in
ICU first 12 hours Mediastinal drainage in ICU first 12 hours Coagulation study results
at various sample times Requirement for chest re-exploration Ventilation duration in
ICU Duration of stay in ICU
Inclusion Criteria:
Patients with scheduled cardiac surgery undergoing the following procedures Double
valve replacements or repair. Major thoracic aortic surgery including hypothermic
circulatory arrest or descending aortic reconstruction.
Valve repair or replacement in the setting of endocarditis Complex procedures requiring
cardiopulmonary bypass duration anticipated to exceed 180 minutes in patients aged ³70
years
Exclusion Criteria:
Patient unable to give informed consent Patient refusal Allergy to rVIIa Allergy to
aprotinin or prior exposure within 6 months Pre-existing congenital coagulopathy
Pre-existing hypercoagulable state Patients in inclusion criteria whose actual bypass
time does not exceed 180 minutes Unresolved surgical bleeding
Withdrawal from Trial:
At the discretion of treating physicians if the proposed transfusion protocol post CPB
is inadequate to keep up with blood loss a patient can be withdrawn from the trial.
Transfusion therapy according to current medical practice at the discretion of treating
physicians will follow. rVIIa as per current hospital guidelines will be available.
Data will still be collected in this group.
Randomization Pharmacy will randomise patient after notified of entry into study.
Blinded packaged trial medication will be sent to theatre.
Surgical management Surgical technique will be at the discretion of treating surgeon
but techniques that may affect haemostasis (eg. Use of biologic glues etc) will be
recorded.
Anaesthetic management Choice of anaesthetic agents will be at the discretion of
treating anaesthetist.
All patients will receive aprotinin 2 x 106 IV over 1 hour after test dose of 10,000
units over 5 minutes and 2 x 106 IV in the CPB circuit prime. 0.75 x 106 IV to infusion
per hour.
All patients will be haemofiltered on bypass.
Core temperature monitoring on all patients. Standard technique to preserve patient
temperature. Topical head cooling will be used if hypothermic circulatory arrest is
needed.
Cardiopulmonary bypass management
Standardised CPB prime and circuits Cell saver for all patients Cardiotomy return for
all patients
Haemoglobin maintained between 6-8gm/dL during bypass. Aim for haemoglobin of 10gm/dL
at time of weaning from bypass. Units of packed cells transfused on bypass will be
recorded.
Adequate rewarming core temp > 35° for 20 minutes.
Alpha stat pH management. Acid-base pH 7.3-7.5, BE +/- 3 prior to weaning from bypass.
Post bypass period
Transfusion and trial medication administration guidelines are found on Flow Chart.
Red Cell Transfusion Trigger Aim for haemoglobin concentration between 80 and 100
grams/litre using either banked or washed red cells.
The planned “conventional therapy “ of aprotinin and an initial administration
predominately platelets (10 units), cryoprecipitate 3 mls/kg (high concentration of
fibrinogen) and a moderate dose of fresh frozen plasma 5ml/kg is appropriate based on
both our clinical experience and advice from the Australian Red Cross.
If at anytime adherence to protocol at the discretion of treating medical staff is
considered to place the patient at risk of inadequate transfusion, the patient can be
withdrawn and transfusion commenced as determined by medical staff. Data will still be
collected for these patients.
The duration of protocol during transfusion is two hours. Either adequate haemostasis
will have been achieved by the interventions as indicated in the protocol or the
scenario of inadequate haemostasis despite two administrations of standardising
coagulation factor and trial medications followed by open label administration of rVIIa
will have evolved. If this is the case, ongoing transfusion, surgical and medical
management will be at the discretion of medical staff. Administration of rVIIa can be
considered after discussion with trial investigators. Data will still be collected for
such patients.
ICU Management Blood loss measurement in the closed drainage system must be documented
at least once hourly, or more frequently if blood loss is excessive. The patient should
be sat up in bed on arrival in ICU (this will allow CXR to be taken), before starting
to measure drainage. On arrival to ICU coagulation studies should be performed and
repeated 4 hours and 12 hours post arrival. .
Postoperative transfusion according to established ICU protocol Blood loss > 250mL/hr
NOTIFY SURGEON (CONSIDER RETURN TO THEATRE)
CONSISTANT WITH CURRENT PRACTICE: - NO ADMINISTRATION OF rVIIa IN ICU
Re-exploration for bleeding Any patient returning to theatre will be treated at the
discretion of medical staff involved. The administration of rVIIa can be considered
according to current guidelines. Administration of coagulation products at discretion
of treating doctors.
Randomisation will be co-ordinated and supervised by the Trial Pharmacy at the Austin
Hospital.
Due to the expense of the drug, instability in solution and the lack of availability of
a similarly packaged placebo, the mechanism to “blind” medical staff in theatre will
involve an independent registered nurse preparing the drug in an opaque syringe
according to a sealed envelope indicating placebo or trial drug. Randomisation will be
site specific for both the Austin Hospital and Warringal Private Hospital.
Pharmacy will be notified when consent is obtained for a patient. Two doses or rVIIa
will need to be sent to theatre. This will be stored in the blood fridge. Any unused
drug will be returned to Pharmacy with full documentation of drug handling. Nursing
staff involved in trial medication preparation will be educated regarding the necessity
of not revealing whether actual drug or placebo was used.
Statistics
Power Analysis Based on our pilot data we anticipate 80% or more of the group receiving
rVIIa will achieve haemostasis adequate for chest closure without any further
intervention to improve coagulation. (Our primary endpoint) We conservatively estimate
that only 30% or less of placebo group will achieve haemostasis adequate for chest
closure without any further intervention to improve coagulation. Assuming a p value of
< 0.5 and power of 0.8 analysis indicates that to show a 50% difference between groups
34 subjects are needed (17 in each arm). To allow for any withdrawals we plan to enrol
40 patients in the study. Based on current drug usage, the recruitment will take 2
years.
Results Analysis Primary endpoints will be assessed by chi-squared analysis. Secondary
endpoints parametric and non-parametric analysis as appropriate. No interim analysis is
planned. Subgroup analysis according to procedure and surgeon will be performed.
Bias Because of the small number of subjects in this trial, bias may be a problem.
Unequal distribution of each of the four procedures may occur and influence results.
The trial drug is thought to treat coagulopathic bleeding. Any superimposed surgical
bleeding may cause bias.
Adverse Events Patients undergoing cardiac surgery represent a population at relatively
high risk of a range of perioperative complications inherent to their underlying
disease, co-morbidities and the nature of the surgery being undertaken. In the pilot
study the mortality rate was 25 %. It is not intended to report the occurrence all of
these events to the Human Research and Ethics Committee. Any adverse events that do
arise specifically in relation to the conduct of the proposed study will be reported to
the Committee
Feasibility Our pilot series of 40 cases from 2 centres was collected over a 24-month
period. Assuming similar workloads and the addition of another centre ( Alfred
Hospital) recruitment should be completed in 24 months.
HREC approval has been granted by Austin Health for the Austin site. The same HREC is
considering approval for the Warringal Private Hospital site, and the Alfred hospital
will be seeking similar approval from its own HREC.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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