The Clinical Impact of the C0/D Ratio and the CYP3A5 Genotype on Outcome in Tacrolimus Treated Kidney Transplant Recipients

Teun van Gelder; Soufian Meziyerh; Jesse J Swen; Aiko P J de Vries; Dirk Jan A R Moes

doi:10.3389/fphar.2020.01142

The Clinical Impact of the C₀/D Ratio and the CYP3A5 Genotype on Outcome in Tacrolimus Treated Kidney Transplant Recipients

Front Pharmacol. 2020 Jul 31:11:1142. doi: 10.3389/fphar.2020.01142. eCollection 2020.

Authors

Teun van Gelder¹, Soufian Meziyerh^{2

3}, Jesse J Swen¹, Aiko P J de Vries^{2

3}, Dirk Jan A R Moes¹

Affiliations

¹ Department of Clinical Pharmacy & Toxicology, Leiden University Medical Center, Leiden, Netherlands.
² Department of Internal Medicine, Division of Nephrology, Leiden University Medical Center, Leiden, Netherlands.
³ Leiden Transplant Center, Leiden University Medical Center, Leiden, Netherlands.

Abstract

Tacrolimus is metabolized by CYP3A4 and CYP3A5 enzymes. Patients expressing CYP3A5 (in Caucasian patients about 15% of the population but more frequent in African Americans and Asians) have a dose requirement that is around 50% higher than non-expressers to reach the target concentration. CYP3A5 expressers can be considered fast metabolizers. The trough concentration/dose (C₀/D) ratio of tacrolimus has recently been proposed as a prognostic marker for poor outcome after kidney transplantation. Patients with a low C₀/D ratio (also referred to as fast metabolizers) seem to have more tacrolimus-related nephrotoxicity, more BK-viremia, and a lower graft survival. At first sight, the expression of CYP3A5 and a low C₀/D ratio seem to be overlapping factors, both pointing towards patients in whom a higher tacrolimus dose is needed to reach the tacrolimus target concentration. However, there are important differences, and these differences may explain why the impact of the C₀/D ratio on long term outcome is stronger than for CYP3A5 genotype status. Patients with a low C₀/D ratio require a high tacrolimus dose and are exposed to high tacrolimus peak concentrations. The higher peak exposure to tacrolimus (and/or its metabolites) may explain the higher incidence of nephrotoxicity, BK-viremia and graft loss. A potential confounder is the concurrent maintenance treatment of corticosteroids, as steroids are sometimes continued in patients at high immunological risk. Steroids induce the metabolism of tacrolimus via pregnane X receptor mediated increased CYP3A4 expression, resulting in lower tacrolimus C₀/D ratio in high risk patients. Also non-adherence may result in lower C₀/D ratio which is also associated with poor outcome. The C₀/D ratio of tacrolimus does seem to identify a group of patients with increased risk of poor outcome after kidney transplantation. Our recommendation is to monitor tacrolimus peak concentrations in these patients, and if these are high then target slightly lower pre-dose concentrations. Another possibility would be to switch to a prolonged release formulation or to dose the drug more frequently, in smaller doses, to avoid high peak concentrations.

Keywords: CYP3A5; kidney; pharmacogenetics; tacrolimus; transplantation.

Publication types

Review