Prediction of the Impact of <i>CYP2C19</i> Polymorphism on Drug-Drug Interaction between Voriconazole and Tacrolimus Using Physiologically-Based Pharmacokinetic Modelling

Jin, Zhi-Ping; Yan, Miao; Li, Si-Ze; Wang, Bao-Qing; Xu, Qing; Wu, Wei; Li, Xiao-Yu; Lv, Qian-Zhou; Xiang, Xiao-Qiang

doi:10.1590/s2175-97902023e21343

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Article • Braz. J. Pharm. Sci. 59 • 2023 • https://doi.org/10.1590/s2175-97902023e21343 copy

Prediction of the Impact of CYP2C19 Polymorphism on Drug-Drug Interaction between Voriconazole and Tacrolimus Using Physiologically-Based Pharmacokinetic Modelling

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Voriconazole increases tacrolimus blood concentration significantly when coadministrated. The recommendation of reducing tacrolimus to 1/3 in voriconazole package insert seems not to be satisfactory in clinical practice. In vitro studies demonstrated that the magnitude of inhibition depends on the concentration of voriconazole, while voriconazole exposure is determined by the genotype status of CYP2C19. CYP2C19 gene polymorphism challenges the management of drug-drug interactions(DDIs) between voriconazole and tacrolimus. This work aimed to predict the impact of CYP2C19 polymorphism on the DDIs by using physiologically based pharmacokinetics (PBPK) models. The precision of the developed voriconazole and tacrolimus models was reasonable by evaluating the pharmacokinetic parameters fold error, such as AUC_0-24, C_max and t_max. Voriconazole increased tacrolimus concentration immediately in all population. The simulated duration of DDIs disappearance after voriconazole withdrawal were 146h, 90h and 66h in poor metabolizers (PMs), intermediate metabolizers (IMs) and extensive metabolizers(EMs), respectively. The developed and optimized PBPK models in this study can be applied to assit the dose adjustment for tacrolimus with and without voriconazole.

Keywords:
Voriconazole; Tacrolimus; CYP2C19 gene polymorphism; Physiologically based pharmacokinetics (PBPK) model; Drug-drug interaction

Parameters		Input Valuea
Physicochemical properties
MW(g/mol)		349
log P _o:w		1.8
Compound type		Monoprotic base
pK_a		1.76
B/P		1.229
Fraction unbound		0.42
First order absorption model
f_a		0.96
k_a(h^-1)		1.44
f_u,gut		1
P_app,caco-2(10^-6cm/s)		28.10
Minimal PBPK distribution model
V_SS (L/kg)		1.079
Liver K_p		1
Elimination
In vitro metabolic system Recombinant
Pathway	Pathway 1	Pathway 1	Pathway 2
Enzyme	CYP2C19	CYP3A4	CYP3A4
V_max (pmol/ min/pmol)	3^b	0.21^b	0.10
K_m(μmol/L)	3.5	15	11

CYP2C19 Genotype	AUC0-12(μg·h/mL)			C_max (μg/mL)			Tmax(hr)
CYP2C19 Genotype	Predicted	Observed	Fold error	Predicted	Observed	Fold error	Predicted	Observed	Fold error
EM	19.88	18.8	1.06	2.49	2.8	1.12	1.74	1.5	1.16
IM	30.66	33.6	1.10	3.41	4.0	1.17	1.87	1.5	1.25
PM	69.8	67.8	1.03	6.63	7	1.06	2.07	2.8	1.35

Parameters
	predicted	CYP2C19 Genotype
		EM		IM		PM
		observed	FE	observed	FE	observed	FE
AUC_0-24(ng∙h/mL)	108.239	88.3	1.23	108.2	1	94.8	1.14
C_max (ng/mL)	18.8667	18.3	1.3	20.5	1.09	16.3	1.16
T_max(h)	1.41	1.5	1.06	1.7	1.21	1.8	1.28

CYP2C19 Genotype	AUC0-24(ng·h/mL)			Cmax (ng/mL)			Tmax(h)
CYP2C19 Genotype	Predicted	Observed	Fold error	Predicted	Observed	Fold error	Predicted	Observed	Fold error
EM	328.03	389.5	1.19	49.38	48.3	1.02	1.39	2.3	1.65
IM	357.70	540.6	1.51	51.29	54.9	1.07	1.43	2.3	1.61
PM	415.4	570.5	1.37	54.74	60.5	1.11	1.46	2.8	1.92

Universidade de São Paulo, Faculdade de Ciências Farmacêuticas Av. Prof. Lineu Prestes, n. 580, 05508-000 S. Paulo/SP Brasil, Tel.: (55 11) 3091-3824 - São Paulo - SP - Brazil
E-mail: bjps@usp.br

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[1] *Correspondence: Q.-Z. Lv. X.-Q. Xiang. Department of Clinical Pharmacy. School of Pharmacy. Fudan University. 826 Zhangheng Road, Shanghai, 201203, PR China. Phone: 86-21-51980024. E-mail: xiangxq@ fudan.edu.cn.