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CYP3A5*3 and CYP3A4*22 Cluster Polymorphism Effects on LCP-Tac Tacrolimus Exposure: Population Pharmacokinetic Approach
被引:4
作者:

Ali, Zeyar Mohammed
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h-index: 0
机构:
Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain
Univ Barcelona, Sch Pharm, Dept Pharm & Pharmaceut Technol & Phys Chem, Biopharmaceut & Pharmacokinet Unit, Barcelona 08007, Spain Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain

Meertens, Marinda
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h-index: 0
机构:
Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain
Univ Barcelona, Sch Pharm, Dept Pharm & Pharmaceut Technol & Phys Chem, Biopharmaceut & Pharmacokinet Unit, Barcelona 08007, Spain Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain

Fernandez, Beatriz
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h-index: 0
机构:
Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain
Univ Barcelona, Sch Pharm, Dept Pharm & Pharmaceut Technol & Phys Chem, Biopharmaceut & Pharmacokinet Unit, Barcelona 08007, Spain Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain

Fontova, Pere
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Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain

Vidal-Alabro, Anna
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Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain

Rigo-Bonnin, Raul
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Hosp Univ Bellvitge, Biochem Dept, IDIBELL, Barcelona 08908, Spain Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain

Melilli, Edoardo
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Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain

Cruzado, Josep M.
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Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain

Grinyo, Josep M.
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h-index: 0
机构:
Univ Barcelona, Dept Clin Sci, Med Unit, E-08007 Barcelona, Spain Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain

Colom, Helena
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h-index: 0
机构:
Univ Barcelona, Sch Pharm, Dept Pharm & Pharmaceut Technol & Phys Chem, Biopharmaceut & Pharmacokinet Unit, Barcelona 08007, Spain Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain

Lloberas, Nuria
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h-index: 0
机构:
Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain
机构:
[1] Hosp Univ Bellvitge, Nephrol Dept, IDIBELL, Barcelona 08908, Spain
[2] Univ Barcelona, Sch Pharm, Dept Pharm & Pharmaceut Technol & Phys Chem, Biopharmaceut & Pharmacokinet Unit, Barcelona 08007, Spain
[3] Hosp Univ Bellvitge, Biochem Dept, IDIBELL, Barcelona 08908, Spain
[4] Univ Barcelona, Dept Clin Sci, Med Unit, E-08007 Barcelona, Spain
关键词:
Tacrolimus;
LCP-Tac;
population pharmacokinetics;
ABCB1;
renal transplantation;
stable adult patients;
immunosuppression;
EXTENDED-RELEASE TACROLIMUS;
TWICE-DAILY TACROLIMUS;
CLINICAL PHARMACOKINETICS;
RENAL-TRANSPLANTATION;
CYP3A5;
GENOTYPE;
KIDNEY;
MODEL;
CLEARANCE;
PHARMACODYNAMICS;
IMPLEMENTATION;
D O I:
10.3390/pharmaceutics15122699
中图分类号:
R9 [药学];
学科分类号:
1007 ;
摘要:
The aim of the study is to develop a population pharmacokinetic (PopPK) model and to investigate the influence of CYP3A5/CYP3A4 and ABCB1 single nucleotide polymorphisms (SNPs) on the Tacrolimus PK parameters after LCP-Tac formulation in stable adult renal transplant patients. The model was developed, using NONMEM v7.5, from full PK profiles from a clinical study (n = 30) and trough concentrations (C-0) from patient follow-up (n = 68). The PK profile of the LCP-Tac formulation was best described by a two-compartment model with linear elimination, parameterized in elimination (CL/F) and distributional (CLD/F) clearances and central compartment (Vc/F) and peripheral compartment (Vp/F) distribution volumes. A time-lagged first-order absorption process was characterized using transit compartment models. According to the structural part of the base model, the LCP-Tac showed an absorption profile characterized by two transit compartments and a mean transit time of 3.02 h. Inter-individual variability was associated with CL/F, Vc/F, and Vp/F. Adding inter-occasion variability (IOV) on CL/F caused a statistically significant reduction in the model minimum objective function MOFV (p < 0.001). Genetic polymorphism of CYP3A5 and a cluster of CYP3A4/A5 SNPs statistically significantly influenced Tac CL/F. In conclusion, a PopPK model was successfully developed for LCP-Tac formulation in stable renal transplant patients. CYP3A4/A5 SNPs as a combined cluster including three different phenotypes (high, intermediate, and poor metabolizers) was the most powerful covariate to describe part of the inter-individual variability associated with apparent elimination clearance. Considering this covariate in the initial dose estimation and during the therapeutic drug monitoring (TDM) would probably optimize Tac exposure attainments.
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