Liver Transplant Clinical Trial
Official title:
An Assessment of Voriconazole Pharmacokinetics and Pharmacogenetics in Liver Transplant Recipients - Pilot Study
A fixed-dosing regimen of voriconazole is routinely used as prophylaxis against aspergillosis in liver transplant patients admitted to the transplant intensive care unit at UPMC. We hypothesize that use of a fixed-dosing regimen of voriconazole will lead to a large degree of variability in drug exposure among liver transplant patients due to: 1) variability in absorption and elimination caused by physiological characteristics unique to this patient population 2) its non-linear pharmacokinetics and 3) the potential for polymorphism in the genes that encode for cytochrome P-450 enzymes that metabolize voriconazole. This is a pilot clinical pharmacokinetic evaluation that will: 1) characterize the plasma concentration versus time profile of voriconazole in liver transplant patients receiving a fixed-dosing regimen to assess for extremes in systemic exposure 2) determine the oral bioavailability of voriconazole in liver transplant patients 3) assess for functionally significant allelic variation of the cytochrome P-450 enzymes that metabolize voriconazole (CYP2C9, CYP2C19 and CYP3A4/5) in both recipient blood and allograft tissue that may contribute extremes in systemic exposure among liver transplant patients. This evaluation will allow for an assessment of the adequacy of the prophylactic regimen in achieving therapeutic drug concentrations in all subjects. Additionally, the utility of genotyping as a clinical tool to identify patients at risk for extremes in voriconazole exposure will be evaluated. The characterization of the pharmacokinetics in liver transplant patients may be utilized to define an optimal therapeutic regimen that will be individualized to target specific concentrations to maximize efficacy and minimize side-effects.
All liver transplant patients receiving voriconazole prophylaxis are eligible to participate
in this study. We propose a single-center, observational study in 15 liver transplant
patients who are admitted to the ICU and receiving voriconazole prophylaxis as part of
standard care. Each patient will undergo blood sampling (27 mL) on one occasion
(Pharmacokinetic Study I), while receiving oral voriconazole. A small portion of blood (1
mL) collected during this blood sampling period will be retained for genotyping (specific
aim III).
Voriconazole prophylaxis is most often administered to liver transplant patients via the
oral route (200 mg twice daily). However, circumstances may arise necessitating the
administration of intravenous doses of voriconazole for a subset of patients, as part of
their standard care. . Thus, these patients will undergo blood sampling on a maximum two
additional occasions: 1) surrounding an intravenous dose dose (27 mL) 2) surrounding an oral
dose (27 mL) .
The amount of voriconazole present in the blood samples will be measured via high pressure
liquid chromatography. Individual plasma concentration time profiles will be determined
following oral and intravenous dosing, respectively. Pharmacokinetic parameter estimates
will be derived via population and individual pharmacokinetic data analysis.
The use, dose, and frequency of the medication voriconazole is up to the clinical staff. We
will not be altering the delivery, dose or use of the drug. Therefore we cannot provide you
with the requested information because it will all depend on the clinical team. We are not
intervening to enroll subjects. Subjects will only be enrolled if they are placed on
voriconazole and they agreed to participate.
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