Clinical Pharmacokinetics and Impact of Hematocrit on Monitoring and Dosing of Tacrolimus Early After Heart and Lung Transplantation

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2020-04

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Sikma, M. A.ORCID 0000-0003-3872-5771ISNI 0000000390805023
Hunault, Claudine CORCID 0000-0001-7843-6208ISNI 0000000396049679
Huitema, Alwin D.R.ISNI 0000000397166009
de Lange, Dylan WORCID 0000-0002-0191-7270
van Maarseveen, EMISNI 0000000396846440

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Abstract

The calcineurin inhibitor tacrolimus is an effective immunosuppressant and is extensively used in solid organ transplantation. In the first week after heart and lung transplantation, tacrolimus dosing is difficult due to considerable physiological changes because of clinical instability, and toxicity often occurs, even when tacrolimus concentrations are within the therapeutic range. The physiological and pharmacokinetic changes are outlined. Excessive variability in bioavailability may lead to higher interoccasion (dose-to-dose) variability than interindividual variability of pharmacokinetic parameters. Intravenous tacrolimus dosing may circumvent this high variability in bioavailability. Moreover, the interpretation of whole-blood concentrations is discussed. The unbound concentration is related to hematocrit, and changes in hematocrit may increase toxicity, even within the therapeutic range of whole-blood concentrations. Therefore, in clinically unstable patients with varying hematocrit, aiming at the lower therapeutic level is recommended and tacrolimus personalized dosing based on hematocrit-corrected whole-blood concentrations may be used to control the unbound tacrolimus plasma concentrations and subsequently reduce toxicity.

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Sikma, M A, Hunault, C C, Huitema, A D R, De Lange, D W & Van Maarseveen, E M 2020, 'Clinical Pharmacokinetics and Impact of Hematocrit on Monitoring and Dosing of Tacrolimus Early After Heart and Lung Transplantation', Clinical Pharmacokinetics, vol. 59, no. 4, pp. 403-408. https://doi.org/10.1007/s40262-019-00846-1