Miniatura

Fitxers

818895.pdf (2.09 MB)

Tipus de document

Article

Versió

Versió publicada

Data de publicació

2017-06-08

Llicència de publicació

cc-by (c) Woillard, J.B. et al., 2017
Si us plau utilitzeu sempre aquest identificador per citar o enllaçar aquest document: https://hdl.handle.net/2445/220251

Tacrolimus updated guidelines through popPK modeling: how to benefit more from CYP3A pre-emptive genotyping prior to kidney transplantation

Títol de la revista

Autors

Director/Tutor

ISSN de la revista

Títol del volum

Recurs relacionat

https://doi.org/10.3389/fphar.2017.00358

Resum

Tacrolimus (Tac) is a profoundly effective immunosuppressant that reduces the risk of rejection after solid organ transplantation. However, its use is hampered by its narrow therapeutic window along with its highly variable pharmacological (pharmacokinetic [PK] and pharmacodynamic [PD]) profile. Part of this variability is explained by genetic polymorphisms affecting the metabolic pathway. The integration of CYP3A4 and CY3A5 genotype in tacrolimus population-based PK (PopPK) modeling approaches has been proven to accurately predict the dose requirement to reach the therapeutic window. The objective of the present study was to develop an accurate PopPK model in a cohort of 59 kidney transplant patients to deliver this information to clinicians in a clear and actionable manner. We conducted a non-parametric non-linear effects PopPK modeling analysis in Pmetrics®. Patients were genotyped for the CYP3A4∗22 and CYP3A5∗3 alleles and were classified into 3 different categories [poor-metabolizers (PM), Intermediate-metabolizers (IM) or extensive-metabolizers (EM)]. A one-compartment model with double gamma absorption route described very accurately the tacrolimus PK. In covariate analysis, only CYP3A genotype was retained in the final model (Δ-2LL = -73). Our model estimated that tacrolimus concentrations were 33% IC95%[20-26%], 41% IC95%[36-45%] lower in CYP3A IM and EM when compared to PM, respectively. Virtually, we proved that defining different starting doses for PM, IM and EM would be beneficial by ensuring better probability of target concentrations attainment allowing us to define new dosage recommendations according to patient CYP3A genetic profile.

Matèries

Farmacocinètica, Immunosupressors, Trasplantament renal, Posologia

Matèries (anglès)

Pharmacokinetics, Immunosupressive agents, Kidney transplantation, Posology

Citació

Col·leccions

Articles publicats en revistes (Infermeria Fonamental i Clínica)

Citació

HESSELINK, Dennis a., WOILLARD, Jean-baptiste, MOURAD, Michel, NEELY, Michael, CAPRON, Arnaud, VAN SCHAIK, Ron h., VAN GELDER, Teun, LLOBERAS BLANCH, Núria, MARQUET, Pierre, HAUFROID, Vincent, ELENS, Laure. Tacrolimus updated guidelines through popPK modeling: how to benefit more from CYP3A pre-emptive genotyping prior to kidney transplantation. _Frontiers in Pharmacology_. 2017. Vol. 8, núm. 358-364. [consulta: 24 de gener de 2026]. ISSN: 1663-9812. [Disponible a: https://hdl.handle.net/2445/220251]

Exportar metadades

JSON - METS

Compartir registre