Platelet Dysfunction Clinical Trial
Official title:
The Influence of Drugs Routinely Used in Cardiac Anesthesia on Impedance Aggregometry.
Impedance aggregometry (IA) (Multiplate®)is a new whole blood platelet function test with potential use in anesthesia and intensive care. Most anesthetic drugs have been shown to have in vitro antiplatelet activity. The goal of this in vitro study is to evaluate the effect of several drugs, frequently used in cardiac anesthesia and intensive care, on platelet function as measured by IA
Impedance aggregometry (IA) on the multiple platelet function analyzer (Multiplate®) ) is a
whole blood point of care test evaluating platelet function. In IA, the increase in
electrical impedance of whole blood is measured after the addition of a platelet activator.
Some of the activators available are arachidonic acid (ASPI Test), ADP (ADP Test), TRAP-6
(TRAP Test) and collagen (COL TEST).
When an activator is added to the blood sample, the activated platelets will aggregate on
the electrodes embedded in the test recipient. As platelets accumulate on the electrodes
surface, the impedance will increase. The increase is measured and expressed in arbitrary
units (AU). Reduced impedance implies platelet dysfunction or the presence of specific
platelet inhibitors. For example, the ASPI test is inhibited in the presence of
acetylsalicylic Acid and clopidrel inhibits the ADP test. Thrombin (TRAP) is an extremely
potent agonist which can be used to monitor GpIIb/IIIa therapy.
The Multiplate® analyzer may have an important role in detecting and analyzing perioperative
coagulopathies, but many drugs, routinely used in cardiac anesthesia or in the intensive
care unit, have known in vitro antiplatelet effects, and may interfere with IA
interpretation.
The goal of the study is to evaluate the influence of lidocaine, propofol, midazolam, and
magnesium on the results of impedance aggregometry and to understand to which extent the
tests are modified by the presence of one of these drugs.
20 healthy volunteers aged 18 to 65 years old will be recruited. Exclusion criteria are the
use of non-steroidal anti-inflammatory drugs for 2 weeks prior to donation and known
coagulation disorders. Whole blood is taken from the antecubital vein. Platelet count is
measured. Blood samples for Multiplate® analysis are drawn in hirudin anticoagulated tubes.
During storage, blood is gently moved in order to avoid sedimentation and spontaneous
platelet aggregation.
For each sample baseline measurements are performed using ASPI Test, ADP Test, TRAP Test and
COL Test.
The four study drugs are added to the blood samples, in isovolumic dilutions, to obtain
subclinical, normal or near toxic plasma concentrations (table 1).
Study drugs low intermediate high Lidocaine (mcg/ml) 1 3 6 Magesium (mMol/l) 0.4 1 2.5
Midazolam (ng/ml) 150 250 500 Propofol (mcg/ml) 2 5 8 Table 1. Plasma concentration of the
four study drugs
For every concentration, IA is measured using the 4 different activators. For every test and
dose, the area under the curve is compared with the baseline.
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