Your search keyword '"Voclosporin"' showing total 4 results

1. Cytochrome P450 3A and P-glycoprotein drug-drug interactions with voclosporin.

Author

Ling, Spencer Y., Huizinga, Robert B., Mayo, Patrick R., Larouche, Richard, Freitag, Derrick G., Aspeslet, Launa J., and Foster, Robert T.

Subjects

*CYTOCHROME P-450, *LUPUS nephritis, *DRUG interactions, *MIDAZOLAM, *KETOCONAZOLE, *THERAPEUTICS

Abstract

Aims Voclosporin is a novel calcineurin inhibitor intended for prevention of organ graft rejection and treatment of lupus nephritis. Pharmacokinetic drug interactions between voclosporin and a CYP3A inhibitor, inducer and substrate and a P-glycoprotein inhibitor and substrate were evaluated. Methods Voclosporin 0.4 mg kg−1 was administered to 24 subjects in each of five studies, as follows: every 12 h ( Q12H) alone and concomitantly with ketoconazole 400 mg once daily ( QD); single dose before and single dose after rifampin 600 mg QD; Q12H where midazolam 7.5 mg was administered as a single dose alone before voclosporin and with last the dose of voclosporin; Q12H alone and concomitantly with verapamil 80 mg every 8 h; and Q12H with digoxin 0.25 mg QD. The noncompartmental pharmacokinetic parameters maximal concentration ( Cmax) and area under the concentration-time curve ( AUC) were obtained, and geometric least squares mean ratios and 90% confidence intervals were evaluated. Results Ketoconazole increased voclosporin Cmax (6.4-fold) and AUC (18-fold); rifampin reduced voclosporin AUC (0.9-fold); voclosporin did not change exposure of midazolam or α-hydroxy-midazolam; verapamil increased voclosporin Cmax (2.1-fold) and AUC (2.7-fold); and voclosporin increased digoxin Cmax (0.5-fold), AUC (0.25-fold) and urinary excretion (0.2-fold). Conclusions Administration of voclosporin concomitantly with strong inhibitors and inducers of CYP3A resulted in increased and decreased exposures, respectively, and should be considered contraindicated. Drug-drug interactions involving voclosporin and CYP3A substrates are not expected. Administration of voclosporin concomitantly with inhibitors and substrates of P-glycoprotein resulted in increased voclosporin and substrate exposures, respectively. Appropriate concentration and safety monitoring is recommended with co-administration of voclosporin and P-glycoprotein substrates and inhibitors. [ABSTRACT FROM AUTHOR]

Published

2014

2. Population PKPD of voclosporin in renal allograft patients.

Author

Mayo, P.R., Ling, S.Y., Huizinga, R.B., Freitag, D.G., Aspeslet, L.J., and Foster, R.T.

Subjects

*BIOMARKERS, *CONFIDENCE intervals, *GOODNESS-of-fit tests, *HOMOGRAFTS, *IMMUNOSUPPRESSIVE agents, *KIDNEY transplantation, *RESEARCH funding, *DATA analysis software, *STATISTICAL models, *DESCRIPTIVE statistics

Abstract

The aims of this population-pharmacokinetic/pharmacodynamic (POP-PKPD) analysis of voclosporin in renal allograft patients were to build a POP-PKPD model for voclosporin and calcineurin activity (CNa) and identify clinically relevant covariates that could assist dosing of the drug. POP-PKPD modeling was performed using a stochastic approximation of the standard expectation maximization (SAEM) algorithm for nonlinear mixed-effects as implemented in Monolix™ 3.2. Voclosporin whole blood concentrations were obtained from de novo renal allograft patients and assayed using a validated LC/MS/MS assay. CNa was measured using a 32P-radiolabeled assay. A two-compartment model with simultaneous sigmoid inhibitory Emax model was used to describe the PKPD relationship between voclosporin concentration and CNa. The POP-PKPD model was then utilized to simulate an optimal initial dosing strategy. Eighty-seven patients were included in the POP-PKPD study. Population mean estimates (relative standard error, rse) for oral clearance (CL/F) and first compartment volume of distribution (V1), were 717 mL min−1 (35%) and 2010 mL (17%), respectively. Maximum CNa Inhibition (Imax), effective concentration (C50), and baseline immunosuppression (S0) were 0.87 pmol/min/mg (8.0%), 123 ng/mL (10%), and 1.15 pmol/min/mg (4.0%), respectively. Covariate analyses demonstrated that age and body surface area significantly influenced CL/F: [ABSTRACT FROM AUTHOR]

Published

2014

3. Pharmacokinetics of voclosporin in renal impairment and hepatic impairment.

Author

Ling, S.Y., Huizinga, R.B., Mayo, P.R., Freitag, D.G., Aspeslet, L.J., and Foster, R.T.

Subjects

*ANALYSIS of variance, *AUTOIMMUNE diseases, *CONFIDENCE intervals, *HYDROLASES, *IMMUNOSUPPRESSIVE agents, *KIDNEYS, *LIVER, *MEDICAL cooperation, *REGRESSION analysis, *RESEARCH, *T-test (Statistics), *DATA analysis software, *DESCRIPTIVE statistics, *CHEMICAL inhibitors

Abstract

Voclosporin is a novel calcineurin inhibitor intended for prevention of organ graft rejection and treatment of lupus nephritis. These studies evaluated the effect of renal or hepatic impairment on pharmacokinetics of voclosporin. Thirty-three subjects were enrolled into 1 of 4 groups based on renal function as defined by creatinine clearance and 18 subjects were enrolled into 1 of 3 groups based on hepatic function defined by Child-Pugh classes. Voclosporin 0.4 mg/kg was administered orally. Geometric mean ratios (renal/hepatic impairment-to-normal) and 90% confidence intervals for Cmax and AUC were calculated. A default no-effect interval of 80-125% was set. Although 90% confidence intervals exceeded the no-effect intervals for both parameters, individual Cmax and AUC plots indicate almost complete overlapping range of values for mild and moderate renal impairment and normal subjects. Severe renal impairment resulted in a 1.5-fold increase in AUC without an increase in Cmax. Mild to moderate hepatic impairment resulted in a 1.5- to 2-fold increase in voclosporin exposure. Voclosporin can be administered safely to patients with mild to moderate renal impairment without dose modification. Appropriate safety monitoring with concentration-based adjustments in transplantation are recommended for patients with severe renal impairment, and for patients with hepatic impairment. [ABSTRACT FROM AUTHOR]

Published

2013

4. Voclosporin Food Effect and Single Oral Ascending Dose Pharmacokinetic and Pharmacodynamic Studies in Healthy Human Subjects.

Author

Mayo, Patrick R., Huizinga, Robert B., Ling, Spencer Y., Freitag, Derrick G., Aspeslet, Launa J., and Foster, Robert T.

Subjects

*ANALYSIS of variance, *CONFIDENCE intervals, *CYCLOSPORINE, *DRUG-food interactions, *GRAFT rejection, *LONGITUDINAL method, *MATHEMATICAL statistics, *REGRESSION analysis, *RESEARCH funding, *LUPUS nephritis, *PARAMETERS (Statistics), *RANDOMIZED controlled trials, *BLIND experiment, *DATA analysis software, *STATISTICAL models, *DESCRIPTIVE statistics, *PHARMACODYNAMICS

Abstract

Voclosporin (VCS) is a novel calcineurin (CN) inhibitor intended for prevention of organ graft rejection and treatment of lupus nephritis. These studies evaluated the single ascending dose pharmacokinetics (PK) and pharmacodynamics (PD, CN activity) of VCS and the effect of food. VCS was administered orally in single doses of 0.25 through 4.5 mg/kg in 62 subjects in the single ascending dose study and as a single oral 1.5 mg/kg dose to 18 subjects after fasting, consumption of a low-fat and high-fat meal. Non-compartmental PK, PD, and PKPD correlation were evaluated. Following single oral doses, systemic exposure increased in a linear manner and demonstrated 1:1 dose-proportional, first-order linear PK above 1.5 mg/kg. VCS inhibited CN activity in a dose-related fashion with maximal inhibition peaking at 3.0 mg/kg. PKPD correlation indicated an EC50 of 78.3 ± 6.8 ng/mL. Administration of VCS with a low-fat and high-fat meal decreased Cmax by 29% and 53%, respectively, and AUCinf by 15% and 25%, respectively. Following ascending single doses of VCS, exposure increased in a linear fashion. A food effect on exposure was demonstrated, with a more pronounced effect following a high-fat meal. VCS concentrations were also found to correlate with CN activity. [ABSTRACT FROM AUTHOR]

Published

2013