Cardiac Event Clinical Trial
Official title:
Pharmacokinetics of Post Operative Cefuroxime in Infants Undergoing Cardiac Surgery
- To evaluate plasma concentrations of Cefuroxime in this patient population
- To determine if certain pathophysiological and/or iatrogenic conditions alter the
pharmacokinetics in this patient group.
- To develop a rational physiological population pharmacokinetic model that describes
plasma concentrations of medications in these patients.
Congenital heart defects are structural or functional anomalies in the heart that occur
during fetal development and are present at birth. Congenital heart disease is the most
common congenital structural malformation. The survival of children born with congenital
heart disease has improved dramatically over the past thirty years, improvements in
diagnosis, medical and surgical management as well as anaesthetic care has improved survival
rates from 20% to 80%.
Paediatric cardiac surgery Children with congenital heart disease may undergo either closed
or open heart surgery. In a closed operation, the heart and main blood vessels can be
operated on while the heart is still beating. In open procedures, the heart is opened and the
blood flow to the child's vital organs is supported by a heart-lung bypass machine
(Cardio-pulmonary bypass - CBP). In light of improving outcomes recent years has seen a
worldwide shift towards neonatal biventricular repair where possible. For those where repair
is not possible then the majority will be offered surgical univentricular palliation
typically requiring 'high-risk' surgery in the first few weeks. 'High risk' neonates
undergoing cardiac surgery often spend prolonged periods on the intensive care requiring
maximal support.
These patients on the intensive care unit can suffer from multi-organ failure due to a
variety of reasons and may require cardiovascular and respiratory support, and also renal
replacement therapy in the form of peritoneal dialysis or haemodialysis/filtration. As a
result of organ failure/support and different cardiac anatomy and physiology, the
pharmacokinetics of drugs used in this post-operative period could potentially vary greatly.
Post-operative surgical site infections Post operative wound infections in paediatric
patients undergoing cardiothoracic surgery occurs in 2.3% to 8% of patients. This
complication results in increased morbidity, longer hospitalisations and increased cost. A
major strategy in reducing postoperative surgical site infections has been the use of
perioperative antibiotics to reduce primarily gram-positive skin flora that colonises the
skin and can potentially infect an open wound.
Of particular concern for patients undergoing cardiac surgery are deep sternal wound
infections or mediastinitis. Associated mortality is significant and has been reported to be
as high as 60% in adults although there is little comparable data for children.
Neonates are at high risk of post-operative sternal wound infection, with an incidence of
5.5% versus 0.5% in older children in one study, which also highlighted an increased
morbidity and mortality in the neonatal group.
Audit and data from our own institution has clarified that children aged less than 3 months
at the time of surgery are at highest risk of developing a post-operative surgical site
infection, and that the most commonly isolated organism is Staphylococcus Aureus.
Cefuroxime is the preferred choice of antibiotic prophylaxis in Alder Hey Children's
Hospital. It is given intra-operatively, and post operatively for 24hours post, unless the
patient's chest remains open, in which case the cefuroxime is continued until the chest is
closed, or they are changed to another anti-microbial.
Pharmacokinetics of drugs in paediatric patients undergoing cardiac surgery Pharmacokinetics
is a discipline aimed at predicting the best dosage and dosing regimen for each single drug
in order to ensure and maintain therapeutically effective concentrations at the action sites.
In postoperative cardiac patients in critical care, there are a number of pathophysiological
and iatrogenic conditions that may significantly alter the pharmacokinetic behavior of drugs.
These include -
- age
- weight
- temperature (if the patient is being actively cooled)
- single/biventricular circulations
- acute kidney injury
- passive peritoneal drainage
- active peritoneal dialysis
- continuous veno-venous haemofiltration/dialysis
- extra-corporeal membrane oxygenation
There is research available that paediatric patients undergoing cardiac surgery with
cardio-pulmonary bypass (CPB) may have sub-therapeutic cefuroxime levels and the dose of
cefuroxime should be adjusted accordingly.
In post op paediatric cardiac patients there are a number of studies describing different
drug pharmacokinetics:
Dexmedetomidine pharmacokinetics may be influenced by age within the neonatal period, weight,
total bypass time, and presence of intracardiac shunt.
Lower bodyweight was associated with lower epinephrine clearance. Milrinone clearance also
appears to increase with age. Phenobarbital pharmacokinetics is also influenced by age and
weight. Subjects with single ventricle physiology demonstrated a 15% decrease in clearance
when compared with subjects with two-ventricle physiology.
So far to date, there are no pharmacokinetic studies investigating cefuroxime in this
specific post-operative patient population.
Moreover, variations in the extracellular fluid content as a response to the trauma of
surgery and the fluid load or significant drug loss through thoracic drainages or through PD
catheter may significantly lower plasma concentrations of extracellularly distributed
hydrophilic antimicrobials (beta-lactams, aminoglycosides and glycopeptides). Instability of
renal function may promote significant changes in body fluid concentrations of renally
eliminated drugs, even in a brief period of hours.
These factors cumulatively may lead to reduced or increased exposure to drugs. Dosages of
some medicines are generally reduced in paediatric population following cardiac surgery to
account for potential AKI (e.g. prophylactic antimicrobials), however potential losses
through PD dialysis or through free drainage via PD catheter are not usually considered.
Passive Peritoneal Drainage/Peritoneal dialysis following paediatric cardiac surgery Children
undergoing surgery for congenital heart disease are especially prone to acute kidney injury
(AKI). It is difficult to appreciate the true incidence of this complication because,
throughout the literature available, great variability is seen in the criteria used for the
diagnosis. The reported incidence ranges between 1% and 17%, depending largely on the
criteria used to define the condition, and the associated mortality is between 21% and 70%.
Peritoneal dialysis is commonly used in the post-operative period after cardiac surgery to
aid the removal of fluids or sometimes as a treatment modality for acute kidney injury.
It is routine clinical practice in many centers, including ours (Department of Cardiac
Surgery at Alder Hey Children's Hospital) to insert a peritoneal dialysis catheter electively
at the time of surgery for potential peritoneal dialysis in neonates and children undergoing
bypass surgery deemed to be at significant risk of needing post-operative PD. Following
elective insertion of a PD catheter, hourly fluid drainage is documented as part of the
routine ICU fluid balance charts. The vast majority will drain some fluid from the catheter
in the initial hours. AKI usually develops early and PD is usually prescribed in the first
days after the operation.
Between January 2014 until March 2015, 420 children underwent cardiac surgery at Alder Hey
children's Hospital. Of these patients, 4% required PD in the post-operative period.
ECMO Occasionally patients are unable to be weaned from cardiopulmonary bypass following
surgery, or deteriorate after arrival to intensive care and require Extracorporeal Membrane
Oxygenation (ECMO). This group of patients have an increased volume of distribution and
therefore, altered pharmacokinetic changes.
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