Cardiac Surgery Clinical Trial
Official title:
Impact of Catecholamine-O-Methyl-Transferase Enzyme Activity on Clinical and Biological Parameters in Patients After Cardiac Surgery.
Although clinical risk factors for postoperative development of vasodilatory shock and acute
renal failure have been identified; there is a considerable proportion of patients
undergoing cardiac surgery where this syndrome cannot be predicted.
We sought to investigate the impact of Catecholamine-O-Methyltransferase (COMT) polymorphism
on the duration of vasodilatory shock and other important clinical outcomes in cardiac
surgery patients.
COMT is a key enzyme in the degradation of catechols eg. catecholamines. 25% of the
population have a low activity (L/L) of this enzyme. Sustained low COMT activity is
associated with an altered metabolic profile of catecholamines and their degradation
products.
The process of cardiopulmonary bypass (CPB)over-activates some of the same mechanisms the
body uses to defend itself against severe infection. One of the main overactive defence
mechanisms is the release of highly toxic compounds derived from oxygen - a process called
'oxidative-stress'. Increased reactive oxygen species (ROS) generation can lead to
inactivation of biologic mediators, including catecholamines. It is well established that
some radicals autoxidizes catecholamines, including DA, NE, and epinephrine and contribute
significantly to vasoplegia.
As part of this study, we will take six 2.7mL samples of blood, collected before, and after
the operation, from the arterial catheter routinely inserted in every patient. This blood
will be used to measure COMT genotype, the concentration of plasma-catecholamines as well as
marker of oxidative stress.
Our plan is to enrol patients undergoing cardiac surgery if the use of the CPB is planned.
Aim of the study
To explore if there is an impact of LL COMT genotype on clinical and biological outcome
variables in patients undergoing cardiac surgery compared to HH genotype.
Background
Cardiac surgery has been shown to be an effective method for prolonging life in patients
with severe coronary artery disease or valvular disease or a combination thereof.
Catechol-O-Methyl-Transferase (COMT) catalyses the O-methylation of biologically active
catechols and is responsible for the degradation of catecholamines and catecholestradiols.
COMT is an intracellular enzyme, which is widely distributed throughout most of all human
tissues (Roth, Maennistoe) Because COMT is expressed ubiquitously, it appears that the COMT
genotype significantly affects levels of catecholamines throughout the body.
25 % of Caucasians are homozygous for low COMT activity, (COMT LL=Met/Met), 25% are
homozygous for high activity of COMT (COMT HH=Val/Val), and about 50% are heterozygous (COMT
HL=Val/Met). (Palmatier, Spielman, Boudikova)
Thus, COMT polymorphism may play an important role in the outcome of patients after cardiac
surgery.
So far, studies due to this polymorphism exist only for chronic, non-cardiac surgery
disorders like psychiatric diseases, breast cancer and alcoholism.
In a prospective observational study, we used this model of CPB-induced stress-mediated
vasodilatory shock to investigate the impact of COMT polymorphism on relevant postoperative
clinical outcomes. Within this model we tested the hypothesis that, in cardiac surgery
patients, the LL COMT genotype is associated with alterations in catecholamine metabolism
and adverse hospital outcomes such as prolonged vasopressor support and acute renal failure
compared to HL and HH COMT genotype.
Patients with a L/L COMT polymorphism are probably used to higher concentrations of
endogenous catecholamines, because a low COMT enzyme activity can cause an impaired
degradation of catecholamines. Patients with a L/L COMT polymorphism require presumably
higher catecholamines support than other patients to maintain cardiovascular stability in
extreme stress-conditions occuring during CPB procedures.
Acute renal failure (ARF) is a common postoperative complication in cardiac surgery patients
that is associated with increased morbidity and mortality. Catechol-O-methyltransferase
(COMT) shows high activity in proximal tubular epithelial cells - target cell in ARF. We
hypothesized that the COMT met158 genotype might be associated with increased risk of acute
renal failure compared to COMT val158 genotype.
CPB activates components of the non-specific immune system, which leads to the generation of
compounds containing oxygen free radicals. A study of 14 patients undergoing cardiac surgery
found increased levels of serum lipid peroxidation products (thiobarbituric acid reactive
substances) within 15 minutes of the commencement of CPB, which returned to preoperative
levels by the following morning. The total serum antioxidative capacity was correspondingly
decreased intraoperatively, and remained decreased at 24 hours postoperatively.
Outcomes will be the length of vasopressor support in patients with LL COMT genotype
compared to patients with HL and HH COMT genotype. We hypothesize that there is a
significant increase in the duration of vasopressor support in patients with LL COMT
compared to patients with HL and HH COMT genotype.
Additional outcome measure and hypotheses
We hypothesize that differences similar to that seen in the duration of vasopressor support
will be seen in a higher proportion of postoperative acute renal failure (increase in serum
creatinine >50% from baseline to peak value), longer duration of ICU and hospital stay in LL
COMT patients compared to HL and HH patients.
COMT genotype will be determined and levels of endogenous catecholamines will be measured
before and after cardiac surgery. We hypothesize that higher levels of endogenous
catecholamines will be measured for patients with LL COMT genotype.
Study Design - overview and rationale
COMT genotype and outcome measurements of patients after cardiac surgery will be analyzed in
this study. Concentrations of plasma catecholamines and important degradation products will
be determined before and after the use of CPB. The duration and dose of postoperative
vasopressor support as well as stay in ICU and stay in hospital will be documented.
Data collection
age, sex, body mass index (BMI), body surface area (BSA, insulin (IDDM) or non-insulin
dependent diabetes mellitus (NIDDM), arterial hypertension, hypercholesterolemia,
preoperative serum creatinine, chronic obstructive pulmonary disease (COPD), smoking status,
peripheral vascular disease (PVD), carotid artery disease, myocardial infarction (MI) or
stroke within last six months, atrial fibrillation (AF), and grade of left ventricular
dysfunction defined by the left ventricular ejection fraction using EuroScore definition.
Pre-operative medication including: platelet inhibitors,
ACE-inhibitors/angiotensin-II-receptor1-antagonists, beta-blocker, calcium channel blocker
and statins.
Intra-operative data on type of cardiac surgery (valvular or coronary artery bypass (CABG),
concomitant or complex cardiac surgery involving the ascending aorta), Redo operation, take
back to operating room, electronically stored MAP and duration of CPB. The intra- and
post-operative use of vasopressor (norepinephrine, epinephrine, phenylephrine, ephedrine,
and metaraminol) and inotropic medications (milrinone, dobutamine)hourly until discharge
from the Intensive Care Unit (ICU). We will note the lowest MAP and the lowest cardiac index
(CI) every 6 hours. Postoperative serum creatinine will be measured daily. Finally, ICU and
hospital length of stay as well as hospital mortality were documented.
Withdrawal The treating clinician will have the right to withdraw the patient from the study
if he or she believes that continued participation is jeopardising the patient's well being.
Ethical Issues Given the potential knowledge for the future the balance of benefits and
risks, we consider it ethical to proceed and seek informed consent. This is not a drug trial
or an interventional trial.
Indemnity This is an investigator-initiated study and is not sponsored by industry. The
investigator is a member of staff at Austin Hospital; the hospital is responsible for
indemnifying the investigator in relation to this study. Warringal Private Hospital will be
responsible for indemnification for patients recruited there.
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