Sedation Clinical Trial
Official title:
Safe Administration of Propofol for Sedation in Children
Advances in health care require that more children are given sedation to allow doctors to
perform investigations or minor procedures. Sedation drugs have traditionally been given
orally (swallowed) by children. However, oral sedation drugs have unpredictable
characteristics, such as duration of sedation, which may result in difficulties performing
the planned procedure.
Anesthetic drugs are now invariably used for sedation in children. These are given through
an IV (skinny plastic tube inserted in to a vein). Propofol (white liquid) is the anesthetic
drug most commonly used for sedation at BC Children's Hospital for sedation. Propofol has
several advantages, including an accurately controllable depth of sedation (how deeply
asleep), minimal effect on the heart and circulation and control of reflexes (e,g coughing)
during the procedure. Propofol also promotes rapid recovery with less sickness and an
earlier return to normal functioning following the procedure.
While propofol has many advantages it can cause respiratory depression (reduced breathing
rate). This reduction in breathing is more common if propofol is given quickly. When your
child is given propofol for their proposed procedure this is performed by a pediatric
anesthesiologist who is skilled in supporting breathing should this be required. If your
child does not participate in this study they will still receive propofol administered by
the anesthesiologist as this is our usual practice. It would be routine to administer the
propofol rapidly and then support breathing for a few minutes. This is very safe in the
hands of an expert anesthesiologist but can be sometimes more risky in other settings where
extensive monitoring and anesthesiologists are not available. This is the setting that
propofol is used in many institutions.
Our goal is to determine how quickly propofol can be given without reducing breathing to the
point that help with breathing is required.
Purpose Advances in minimally invasive radiological and surgical techniques demand that
increasing numbers of children are given sedation or anesthesia to facilitate these
procedures, frequently performed on an out-patient or day-care basis. Most are performed
outside the operating room environment, with intensivists and emergency physicians
administering over 55 % of sedation episodes, and only 19% being performed by
anesthesiologists in North America. It is well documented that risks of complications during
sedation exceed those experienced during the much more controlled environment of general
anesthesia, with a twelve-fold increased risk of mortality when sedation is administered
outside the operating room.
Sedative agents have traditionally been administered orally to children. However,
characteristics of oral sedation drugs, such as unpredictable depth and duration of sedation
resulting from variable drug absorption and prolonged duration of drug effect, have resulted
in both high failure and complication rates. Recently, intravenous (IV) anesthetic drugs
with more accurately titratable and predictable characteristics have gained popularity for a
variety of sedation procedures. Propofol is the most commonly used intravenous agent for
these procedures in North America.
Hypothesis The maximum safe infusion rate for an induction dose of propofol administered to
children for sedation can be reliably predicted. Safety will be optimized by preventing
apnoea whilst minimizing the time for induction of sedation and ensuring an adequate depth
of sedation is achieved.
Justification Propofol is an intravenous (IV) anesthetic agent used for induction and
maintenance of anesthesia in both adults and children. Propofol has several characteristics
favouring its use, including an accurately titratable depth of anesthesia, cardiovascular
stability, suppression of upper airway reflexes, rapid recovery with reduced post-operative
nausea and vomiting and overall earlier return to pre-anesthetic functional state. At lower
doses, propofol may also be used to maintain a level of sedation for radiological imaging or
endoscopic investigations.
While propofol provides many advantages it does cause significant respiratory depression.
Adverse respiratory events have been reported to be similar in both adults and children.
Propofol induced respiratory depression may lead to hypoxemia requiring the provision of
supplemental oxygen by mask and/or manual positive pressure ventilation.8 Artificial
ventilation requires significant expertise and if poorly managed may result in gastric
insufflation, pulmonary aspiration or hypoxia, all of which can lead to devastating
complications such as permanent brain injury or death. The maximum dose or rate of
administration of propofol that causes respiratory depression in children has yet to be
accurately defined. Age specific effects have also not been reported.
Objectives
Primary aim:
•Develop a safe dosing schedule for propofol administration in children that will ensure
spontaneous ventilation is maintained in at least 95% of subjects.
Secondary aim:
•Model the effects of propofol induction administered by intravenous infusion to facilitate
the prediction of dosing schedules for different doses, different end-points in different
clinical scenarios.
Research Method Prospective randomized study. Subjects will be randomly assigned to receive
a predetermined infusion rate for propofol during induction of sedation.
Statistical Analysis A graphical representation of each data point with crossovers will be
produced. Data will be analysed on a per protocol basis using the pooled-adjacent-violators
algorithm to estimate the maximal infusion rate whilst preserving spontaneous ventilation.
We will apply the boot-strap methods implemented by Pace to compute 95 % confidence limits.
The effect of age, will be assessed by performing separate analyses in the age-strata.
To model the ventilatory effects of propofol, we will develop a mathematical model of human
respiratory control. We will base this on the respiratory model proposed by Ursino (Ursino
Model)19-21 which is a three compartment model comprising the lung, brain and tissues for
gas exchange. We will enhance the model to include ventilatory regulation, along with
pharmacokinetic and pharmacodynamic models of propofol including a respiratory effect site.
The identification of suitable parameters for the model will include non-linear fitting of
the clinical data (age, weight, BSA, ventilatory volumes, CO2 excretion, respiratory rate,
and entropy).
;
Allocation: Randomized, Endpoint Classification: Pharmacodynamics Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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