Literature DB >> 28005225

Improved Pharmacokinetics with BAY 81-8973 Versus Antihemophilic Factor (Recombinant) Plasma/Albumin-Free Method: A Randomized Pharmacokinetic Study in Patients with Severe Hemophilia A.

Anita Shah¹, Alexander Solms², Dirk Garmann³, Yvonne Katterle², Verzhiniya Avramova⁴, Stanislav Simeonov⁴, Toshko Lissitchkov⁴.

Abstract

BACKGROUND: BAY 81-8973 is a full-length, unmodified, recombinant human factor VIII (FVIII) for the treatment of hemophilia A.
OBJECTIVE: The aim of this study was to compare the pharmacokinetic (PK) profile of BAY 81-8973 with antihemophilic factor (recombinant) plasma/albumin-free method (rAHF-PFM) PATIENTS/
METHODS: In this phase I, open-label, crossover study, men aged 18-65 years with severe hemophilia A and ≥150 exposure days to FVIII were randomized to receive a single intravenous infusion of 50 IU/kg BAY 81-8973 or rAHF-PFM, followed by crossover to a single infusion of the other treatment. FVIII levels were measured in plasma over 48 h using one-stage and chromogenic assays. PK parameters, including area under the curve from time zero to the last data point (AUClast; primary outcome) and half-life (t ½) were calculated. A population PK model was developed to simulate various treatment scenarios.
RESULTS: Eighteen patients were randomized and analyzed. Using both assays, geometric mean (coefficient of variation [%CV]) AUClast was significantly higher, and t ½ was significantly longer, for BAY 81-8973 versus rAHF-PFM (one-stage, AUClast: 1660 IU·h/dL [29.4] vs. 1310 IU·h/dL [29.0], p < 0.0001; one-stage, t ½: 14.5 [25.7] vs. 11.7 h [27.3], p < 0.0001). Simulations showed that median time to 1 IU/dL was approximately 27% longer for BAY 81-8973 versus rAHF-PFM over doses of 25-50 IU/kg; plasma levels >1 IU/dL could be maintained with 14.4 IU/kg BAY 81-8973 or 39.1 IU/kg rAHF-PFM 3×/week.
CONCLUSIONS: BAY 81-8973 showed a superior PK profile versus rAHF-PFM. The same FVIII trough threshold level could be achieved with lower doses of BAY 81-8973 versus rAHF-PFM. ClinicalTrials.gov: NCT02483208.

Entities: Chemical Disease Gene Species

Keywords: Chromogenic Assay; FVIII Activity; Mean Residence Time; Severe Hemophilia; Trough Level

Mesh：

Substances：

Year: 2017 PMID： 28005225 PMCID： PMC5563350 DOI： 10.1007/s40262-016-0492-2

Source DB: PubMed Journal: Clin Pharmacokinet ISSN： 0312-5963 Impact factor: 6.447

Key Points

Introduction

Treatment of hemophilia A typically requires factor VIII (FVIIII) replacement therapy. In most developed countries with adequate resources, FVIII prophylaxis is standard care for patients with hemophilia A [1, 2]. However, insufficient levels of infused FVIII resulting from suboptimal adherence to prophylaxis or individual differences in FVIII pharmacokinetics (PK) may result in breakthrough bleeding during prophylaxis [3-5]. Although the appropriate level of FVIII to prevent bleeding in individual patients varies [6, 7], increased time spent with low FVIII levels is considered an important determinant of breakthrough bleeding during prophylaxis [8]. Thus, maintenance of FVIII above threshold levels for long periods is perceived to be beneficial. The desired threshold level for a given patient can vary based on the bleeding phenotype, activity level, genetic mutation, and other variables. Hemophilia treaters may target threshold levels of 1, 3, 5, or 10 IU/dL FVIII, or higher, while selecting a dosing regimen for prophylaxis [6-8]. BAY 81-8973 is a full-length, unmodified, recombinant human FVIII that has the same amino acid sequence as Bayer’s sucrose-formulated recombinant FVIII (rFVIII-FS; Kogenate® FS, Bayer, Berkeley, CA, USA) but produced with certain, more advanced manufacturing technologies [9]. The changes and enhancements to the BAY 81-8973 manufacturing process include use of a 20-nm viral filtration step capable of removing small non-enveloped viruses and potential protein aggregates; elimination of human- or animal-derived raw materials from the production process; and use of a new, more robust, and higher productivity cell line developed through introduction of the gene for human heat shock protein 70 [9]. Refinements to the manufacturing process of BAY 81-8973 have resulted in an rFVIII product of high and consistent purity with a consistently high degree of sialic acid capping of N-terminal glycans [9], which may affect the half-life (t ½) of some mammalian proteins [10]. BAY 81-8973 has an improved PK profile compared with rFVIII-FS, including increased area under the curve (AUC), t ½, and mean residence time (MRT), as well as decreased clearance (CL) [9]. The safety and efficacy of BAY 81-8973 for prophylaxis (two to three times per week) and on-demand treatment has been demonstrated in children, adolescents, and adults with severe hemophilia A [11-13]. The objective of the current study was to compare the PK profile of BAY 81-8973 with a marketed full-length rFVIII product, antihemophilic factor (recombinant) plasma/albumin-free method (rAHF-PFM). Data collected using the chromogenic assay were used to develop a population PK (popPK) model for BAY 81-8973 and rAHF-PFM to simulate various treatment scenarios in larger patient populations.

Methods

Patients

Men aged 18–65 years with severe hemophilia A (FVIII <1 IU/dL [%]) previously treated with FVIII for ≥150 exposure days were eligible for inclusion in the study. Patients must have also been able to stop FVIII treatment to complete a ≥3-day washout period before study entry and between treatments. Key exclusion criteria included the presence or history of an FVIII inhibitor (≥0.6 Bethesda units/mL), diagnosis of any bleeding disorders other than hemophilia A, platelet count <75,000/mm3, serum creatinine >2× the upper limit of normal (ULN), and alanine aminotransferase or aspartate aminotransferase >5× the ULN.

Study Design

This was a phase I, single-dose, open-label, randomized, crossover study to compare the PK of BAY 81-8973 with rAHF-PFM (ClinicalTrials.gov identifier: NCT02483208). Patients (N = 18) were randomized according to a computer-generated randomization list to receive a single infusion of 50 IU/kg BAY 81-8973 (Kovaltry®; Bayer, Berkeley, CA, USA) or 50 IU/kg rAHF-PFM (Advate®; Baxalta, Westlake Village, CA, USA), followed by crossover to a single infusion of the other treatment, with washout periods of ≥3 days before each single dose. Both products were administered as 10-min intravenous infusions. Informed consent was provided by the patients, and the protocol was approved by the site’s independent Ethics Committee/Institutional Review Board.

Pharmacokinetic (PK) Assessments

Plasma samples were collected predose and 0.25, 0.5, 1, 3, 6, 8, 24, 30, and 48 h postdose for PK assessments. FVIII levels were measured using the one-stage and chromogenic assays, both of which are commonly used for PK studies conducted using FVIII products [9, 14–17]. For the one-stage assay, plasma concentrations of BAY 81-8973 and rAHF-PFM were determined by a turbidimetric assay with activated partial thromboplastin time measurement on the ACL Advance System (Instrumentation Laboratory, Bedford, MA, USA) against a calibration curve of standard human plasma. The calibration range of the procedure for BAY 81-8973 was from 10.0 IU/L (or 1 IU/dL, lower limit of quantitation [LLOQ]) to 600 IU/L (or 60 IU/dL, upper limit of quantification [ULOQ]). Quality control (QC) samples in the concentration range from 25.0 to 450 IU/L were determined with an accuracy of 96.0–104% and a precision of 7.64–14.0%. The calibration range of the procedure for rAHF-PFM was from 10.0 IU/L (or 1 IU/dL [LLOQ]) to 600 IU/L (or 60 IU/dL [ULOQ]). QC samples in the concentration range from 25.0 to 450 IU/L were determined with an accuracy of 98.1–112% and a precision of 6.37–10.0%. For the chromogenic assay, FVIII activity of BAY 81-8973 and rAHF-PFM was determined in citrate plasma by an enzymatic activity assay with chromogenic readout using a commercially available kit and normal human plasma standard as a calibrator. The calibration range of the procedure for BAY 81-8973 was from 10.0 (LLOQ) to 500 IU/L (ULOQ). QC samples in the concentration range from 25.0 to 375 IU/L were determined with an accuracy of 94.3–106% and a precision of 3.75–7.09%. The calibration range of the procedure for rAHF-PFM was from 10.0 (LLOQ) to 500 IU/L (ULOQ). QC samples in the concentration range from 25.0 to 375 IU/L were determined with an accuracy of 98.8–106% and a precision of 2.65–4.00%. For both methods, samples above the calibration range were diluted with severe hemophilic plasma into the working dilution range before analysis. Dilution linearity and parallelism of QC versus patient samples has been proven during validation of the one-stage and chromogenic assays. The following PK parameters were assessed using data collected from both assays: AUC from time zero to the last data point (AUClast; primary variable), AUC from time zero to infinity (AUCinf), maximum concentration (C max), t ½, CL, MRT, and volume of distribution at steady state (V ss). All parameters were calculated using noncompartmental methods (WinNonlin® software; Pharsight Corporation, Mountain View, CA, USA). AUC was calculated using the log-linear trapezoidal method, and t ½ was calculated using the regression analysis of the linear part of the curve on a semilogarithmic scaled plot.

Population PK (PopPK) Model

A popPK model for BAY 81-8973 and rAHF-PFM was developed based on data obtained by the chromogenic assay. The analysis was conducted using the nonlinear mixed-effect modeling approach as implemented in NONMEM® (version 7, level 2.0; ICON, Hanover, MD, USA). A two-compartment model was used as the structural PK model (ADVAN5) and was parameterized by CL, volume of the central compartment (V1), intercompartmental clearance (Q), and volume of the peripheral compartment (V2). In the first step of the model development process, the PK of BAY 81-8973 and rAHF-PFM were assumed to be identical. In the next step, the model was sequentially redefined by testing whether BAY 81-8973 and rAHF-PFM have statistically significant differences in CL, V1, Q, and/or V2. Because of the small study size, no covariate analysis was conducted. Individual PK parameters were derived from the popPK model and were used to estimate t ½ and predict trough levels for a dose of 30 IU/kg BAY 81-8973 and rAHF-PFM administered twice weekly or three times weekly. Furthermore, the popPK model was used to simulate switching from 30 IU/kg rAHF-PFM twice weekly or three times weekly at steady state to the same dose and dosing frequency of BAY 81-8973.

Simulations

The popPK model was used to assess ‘time to reach’ and ‘time below’ FVIII threshold levels of 1, 3, 5, and 10 IU/dL based on a larger virtual patient population after administration of various doses of BAY 81-8973 or rAHF-PFM. Therefore, steady-state profiles for a virtual population (n = 1000 patients) were simulated. The proportion of patients above these thresholds and the required doses to achieve these thresholds were also compared between the two products.

Statistical Analysis

For statistical analysis of the PK parameters obtained by noncompartmental analysis, a log-normal distribution of the parameters was assumed. Log-transformed parameters were analyzed using analysis of variance (ANOVA), including sequence, patient (sequence), period, and treatment effects. Based on these analyses, point estimates (least squares) means and CIs (90% and 95%) for the BAY 81-8973:rAHF-PFM ratio were calculated by retransformation of the logarithmic data using the intraindividual SD of the ANOVA. A sample size of 16 patients was determined to be sufficient to compare PK based on expected intraindividual coefficients of variation between 12.5% and 20% for C max and AUC from previous studies with BAY 81-8973 and rFVIII-FS. The actual results from our study had intraindividual coefficients of variation of 12% and 6.8% for AUC based on the one-stage and chromogenic assays, respectively, and 10% and 4.9% for C max based on the one-stage and chromogenic assays, respectively.

Results

A total of 18 patients from a single center in Bulgaria were randomized and received single doses of BAY 81-8973 and rAHF-PFM. Mean ± SD age for all patients was 37.3 ± 13.8 years, and all patients were white. Demographic data for all 18 patients are provided in Table 1. All patients completed the study and were analyzed.

Table 1

Baseline demographics and clinical characteristics

	All patients [N = 18]
Age, years
Mean ± SD	37.3 ± 13.8
Median (range)	36 (19–64)
Race [n (%)]
White	18 (100)
Weight, kg
Mean ± SD	75.7 ± 13.7
Median (range)	80.0 (55.0–99.0)
BMI, kg/m²
Mean ± SD	24.5 ± 3.7
Median (range)	26.1 (18.5–28.9)
VWF, %
Mean (range)	123 (68–236)^a
Hemophilic arthropathy [n (%)]	4 (22.2)
HCV infection [n (%)]	14 (77.8)

BMI body mass index, HCV hepatitis C virus, VWF von Willebrand factor, SD standard deviation

aData available for 17 patients

Baseline demographics and clinical characteristics BMI body mass index, HCV hepatitis C virus, VWF von Willebrand factor, SD standard deviation aData available for 17 patients

PK Assessments

The FVIII concentration–time profiles show that at several timepoints, FVIII levels are higher for BAY 81-8973 compared with rAHF-PFM (Fig. 1). Predose FVIII baseline values were similar in patients for both treatments. For the one-stage assay, 3/18 (range <LLOQ to 2.5 IU/dL) and 2/18 (range <LLOQ to 1.5 IU/dL) patients had FVIII levels above the LLOQ for BAY 81-8973 and rAHF-PFM, respectively. For the chromogenic assay, 4/18 (range <LLOQ to 2.8 IU/dL) and 3/18 (range <LLOQ to 2.0 IU/dL) patients had levels above the LLOQ for BAY 81-8973 and rAHF-PFM, respectively. AUClast was significantly higher for BAY 81-8973 compared with rAHF-PFM using the one-stage (1660 vs. 1310 IU·h/dL, p < 0.0001) and chromogenic (2200 vs. 1550 IU·h/dL, p < 0.0001) assays. Similar results were obtained for AUCinf (Table 2). The t ½ was also significantly longer for BAY 81-8973 versus rAHF-PFM using the one-stage (14.5 vs. 11.7 h, p < 0.0001) and chromogenic (13.9 vs. 12.0 h, p < 0.0001) assays (Table 2). Independent of the assay, MRT was significantly higher and CL was significantly lower for BAY 81-8973 compared with rAHF-PFM (all p < 0.0001), while C max was similar for BAY 81-8973 and rAHF-PFM (Table 2).

Fig. 1

Table 2

Pharmacokinetic results following single-dose administration of BAY 81-8973 and rAHF-PFM

	Geometric mean (%CV)		Geometric least squares mean ratio^a (95% CI)	p value
	BAY 81-8973	rAHF-PFM	Geometric least squares mean ratio^a (95% CI)	p value
One-stage assay
AUC_last, IU·h/dL	1660 (29.4)	1310 (29.0)	1.27 (1.18–1.36)	<0.0001
AUC_inf, IU·h/dL	1850 (34.3)	1400 (32.4)	1.32 (1.21–1.44)	<0.0001
C _max, IU/dL	119 (15.7)	116 (18.5)	1.02 (0.95–1.10)	0.51
t _½, h	14.5 (25.7)	11.7 (27.3)	1.23 (1.14–1.33)	<0.0001
Range	9.65–21.4	6.83–17.4	NA
MRT, h	19.5 (27.3)	15.7 (29.0)	1.24 (1.16–1.33)	<0.0001
CL, dL/h/kg	0.027 (34.3)	0.036 (32.4)	0.76 (0.70–0.83)	<0.0001
V _ss, dL/kg	0.53 (19.4)	0.56 (17.3)	0.94 (0.88–1.00)	0.07
Chromogenic assay
AUC_last, IU·h/dL	2200 (23.9)	1550 (27.4)	1.42 (1.36–1.49)	<0.0001
AUC_inf, IU·h/dL	2440 (28.5)	1650 (31.0)	1.48 (1.41–1.55)	<0.0001
C _max, IU/dL	151 (19.9)	153 (17.1)	0.98 (0.95–1.02)	0.32
t _½, h	13.9 (25.1)	12.0 (23.3)	1.16 (1.10–1.23)	<0.0001
Range	9.95–22.2	9.06–17.9	NA
MRT, h	19.2 (27.4)	15.0 (27.9)	1.28 (1.21–1.35)	<0.0001
CL, dL/h/kg	0.021 (28.5)	0.030 (31.0)	0.67 (0.64–0.71)	<0.0001
V _ss, dL/kg	0.39 (19.1)	0.46 (16.7)	0.86 (0.82–0.90)	<0.0001

AUC area under the curve, AUC AUC from time zero to infinity, AUC AUC from time zero to the last data point, CI confidence interval, CL total body clearance, C maximum concentration, CV coefficient of variation, MRT mean residence time, NA not applicable, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method, t half-life, V volume of distribution at steady state

aRatio of BAY 81-8973:rAHF-PFM

FVIII level decay curves after single-dose administration of BAY 81-8973 and rAHF-PFM using the a one-stage assay and b chromogenic assay. FVIII factor VIII, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method Pharmacokinetic results following single-dose administration of BAY 81-8973 and rAHF-PFM AUC area under the curve, AUC AUC from time zero to infinity, AUC AUC from time zero to the last data point, CI confidence interval, CL total body clearance, C maximum concentration, CV coefficient of variation, MRT mean residence time, NA not applicable, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method, t half-life, V volume of distribution at steady state aRatio of BAY 81-8973:rAHF-PFM

PopPK Model and Simulations

The parameter estimates of the popPK model are shown in Table 3. Visual predictive checks showed good agreement between the popPK model and the observed data. Model diagnostics (e.g. goodness-of-fit plots such as conditional weighted residuals and standard errors of parameter estimates) indicated a precise and robust estimation of all model parameters (Fig. 2). The popPK model was used to estimate t ½ and predict individual steady-state trough levels following 30 IU/kg BAY 81-8973 or rAHF-PFM administered twice weekly or three times weekly based on individual PK parameters from the 18 patients in the randomized crossover study. In 16 of 18 patients, t ½ was longer for BAY 81-8973 versus rAHF-PFM (Fig. 3), while in the two remaining patients, t ½ was 12.7 versus 13.1 h and 10.0 versus 10.9 h for BAY 81-8973 and rAHF-PFM, respectively. Trough levels were higher in 17 patients following BAY 81-8973 administered twice weekly compared with rAHF-PFM; for three-times-weekly administration, trough levels were higher in all patients after BAY 81-8973 administration (Fig. 4). Typical concentration–time profiles showing FVIII activity 1 week before and 1 week after a simulated switch in treatment from 30 IU/kg rAHF-PFM twice weekly or three times weekly to BAY 81-8973 at the same dose and dosing frequencies are shown in Fig. 5.

Table 3

Parameter estimates of the population pharmacokinetic model

Parameter	Units	Estimate	RSE^a, %	Description
\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$${\text{CL}}^{\text{KOV}}$$\end{document}CLKOV	dL/h	1.51	7.33	Clearance of BAY 81-8973
\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$$V{1}^{{{\text{KOV}},{\text{ADV}}}}$$\end{document}V1KOV,ADV	dL	23.6	2.76	Central volume of distribution of BAY 81-8973 and rAHF-PFM
\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$$Q^{{{\text{KOV}},{\text{ADV}}}}$$\end{document}QKOV,ADV	dL/h	1.59	5.5	Intercompartmental clearance of BAY 81-8973 and rAHF-PFM
\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$$V{2}^{\text{KOV}}$$\end{document}V2KOV	dL	5.35	12.8	Peripheral volume of distribution of BAY 81-8973
\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$$\Delta {\text{CL}}^{\text{ADV}}$$\end{document}ΔCLADV	%	47.8	8.05	Change in clearance for rAHF-PFM compared with BAY 81-8973
\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$$\Delta V{2}^{\text{ADV}}$$\end{document}ΔV2ADV	%	86.6	23.4	Change in peripheral volume of distribution for rAHF-PFM compared with BAY 81-8973
\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$${\text{IIV}}_{\text{Cl}}$$\end{document}IIVCl	CV %^b	27.2	13.9	Intraindividual variability in clearance
\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$${\text{IIV}}_{{V_{1} }}$$\end{document}IIVV1	CV %^b	7.93	36.9	Intraindividual variability in central volume of distribution
\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$${\text{IIV}}_{{\Delta {\text{Cl}}}}$$\end{document}IIVΔCl	CV %^b	35	27.1	Intraindividual variability in change in clearance
\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$${\text{IOV}}_{{F_{1} }}$$\end{document}IOVF1	CV %^b	10.3	31.7	Intraoccasional variability in bioavailability
\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$$\varepsilon_{\text{prop}}$$\end{document}εprop	CV %^c	5.73	6.84	Proportional residual error

CV coefficient of variation, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method, RSE relative standard error, SQRT square root

aAssessed via bootstrap (n = 500, with 485 successful runs)

bCalculated by SQRT(EXP(variance) − 1) × 100

cCalculated by SQRT(variance) × 100

Fig. 2

FVIII level-time profiles in the population pharmacokinetic model for a BAY 81-8973 and b rAHF-PFM. FVIII factor VIII, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method

Fig. 3

Individual t ½ estimates following a dose of 30 IU/kg rAHF-PFM and BAY 81-8973; a solid line indicates that a switch from rAHF-PFM to BAY 81-8973 leads to an expected increase in t ½ for this patient; a dashed line indicates a decrease in t ½ following a switch to BAY 81-8973. rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method, t half-life

Fig. 4

Pharmacokinetic trough level at steady state following a dose of 30 IU/kg rAHF-PFM and BAY 81-8973; a solid line indicates that a switch from rAHF-PFM to BAY 81-8973 leads to an expected increase in trough levels for this patient; a dashed line indicates a decrease in trough level following a switch to BAY 81-8973. C trough level, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method

Fig. 5

Simulation of a typical steady-state profile of a switch from 30 IU/kg rAHF-PFM to 30 IU/kg BAY 81-8973 a twice weekly and b three times weekly. Shaded areas indicate times when FVIII concentrations are <1 IU/dL for panel a and <3 IU/dL for panel b. FVIII factor VIII, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method

Parameter estimates of the population pharmacokinetic model CV coefficient of variation, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method, RSE relative standard error, SQRT square root aAssessed via bootstrap (n = 500, with 485 successful runs) bCalculated by SQRT(EXP(variance) − 1) × 100 cCalculated by SQRT(variance) × 100 FVIII level-time profiles in the population pharmacokinetic model for a BAY 81-8973 and b rAHF-PFM. FVIII factor VIII, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method Individual t ½ estimates following a dose of 30 IU/kg rAHF-PFM and BAY 81-8973; a solid line indicates that a switch from rAHF-PFM to BAY 81-8973 leads to an expected increase in t ½ for this patient; a dashed line indicates a decrease in t ½ following a switch to BAY 81-8973. rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method, t half-life Pharmacokinetic trough level at steady state following a dose of 30 IU/kg rAHF-PFM and BAY 81-8973; a solid line indicates that a switch from rAHF-PFM to BAY 81-8973 leads to an expected increase in trough levels for this patient; a dashed line indicates a decrease in trough level following a switch to BAY 81-8973. C trough level, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method Simulation of a typical steady-state profile of a switch from 30 IU/kg rAHF-PFM to 30 IU/kg BAY 81-8973 a twice weekly and b three times weekly. Shaded areas indicate times when FVIII concentrations are <1 IU/dL for panel a and <3 IU/dL for panel b. FVIII factor VIII, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method The popPK model was used in simulations to assess FVIII threshold levels following administration of BAY 81-8973 and rAHF-PFM in 1000 virtual patients. Time to reach threshold levels of 1, 3, 5, and 10 IU/dL after a single infusion of BAY 81-8973 or rAHF-PFM was derived from simulated dense profiles. After single-dose administration, the median time to a FVIII level of 1 IU/dL was approximately 27% (approximately 18 h) longer for BAY 81-8973 versus rAHF-PFM over a dose range of 25–50 IU/kg (Table 4). Similar results were obtained for 3, 5, and 10 IU/dL FVIII thresholds. Correspondingly, a substantially higher proportion of patients could maintain trough levels above threshold with the same dose of BAY 81-8973 versus rAHF-PFM (Table 5). Based on these simulations, a higher dose of rAHF-PFM compared with BAY 81-8973 would be needed for 50% of patients to maintain FVIII levels >1 IU/kg (161 vs. 52.4 IU/kg on a twice-weekly regimen; 39.1 vs. 14.4 IU/kg on a three-times-weekly regimen), which equates to an approximately 72 IU/kg higher weekly dose for rAHF-PFM versus BAY 81-8973 (Table 6).

Table 4

Median time to FVIII threshold level after a single intravenous dose (simulation of 1000 patients)

Dose, IU/kg	Threshold level, IU/dL	BAY 81-8973, h (5th and 95th Percentiles)	rAHF-PFM, h (5th and 95th Percentiles)	Ratio^a	Difference^b, h
25	1	80.5 (50.5; 122.5)	62.5 (39.5; 100)	1.29	18
25	3	59 (36.5; 90)	43.5 (26.5; 71)	1.36	15.5
25	5	49 (30; 74.5)	34.5 (24; 57)	1.42	14.5
25	10	34.5 (24; 53)	24 (15; 39)	1.44	10.5
30	1	84.5 (53; 128)	65.5 (42; 104.5)	1.29	19
30	3	63 (38.5; 95.5)	46.5 (28.5; 75.5)	1.35	16.5
30	5	52.5 (32.5; 80)	38 (24; 62)	1.38	14.5
30	10	38.5 (24; 58.5)	26 (15; 43.5)	1.48	12.5
40	1	90 (56.5; 136.5)	71 (45.5; 112.5)	1.27	19
40	3	68.5 (42.5; 104)	51.5 (32; 83.5)	1.33	17
40	5	58.5 (36; 89)	43 (26; 70)	1.36	15.5
40	10	44.5 (27; 67.5)	31 (24; 51)	1.44	13.5
50	1	94.5 (59.5; 143.5)	74.5 (48; 118.5)	1.27	20
50	3	73 (45; 110.5)	55.5 (34.5; 89)	1.32	17.5
50	5	63 (38.5; 95.5)	46.5 (28.5; 75.5)	1.35	16.5
50	10	49 (30; 74.5)	34.5 (24; 57)	1.42	14.5

FVIII factor VIII, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method

aRatio of BAY 81-8973:rAHF-PFM

bDifference of BAY 81-8973 − rAHF-PFM

Table 5

Proportion of patients maintaining FVIII levels above the threshold (simulation of 1000 patients)

Dose, IU/kg	Threshold, IU/dL	2×/week regimen^a			3×/week regimen^b
Dose, IU/kg	Threshold, IU/dL	BAY 81-8973 patients, %	rAHF-PFM patients, %	Ratio^c	BAY 81-8973 patients, %	rAHF-PFM patients, %	Ratio^c
25	1	27.0	6.9	3.91	69.1	34.5	2.00
25	3	4.0	0.5	8.00	28.1	6.8	4.13
25	5	1.1	0	–	11.0	2.2	5.00
30	1	33.6	10.0	3.36	75.1	40.1	1.87
30	3	6.2	1.1	5.64	34.7	10.0	3.47
30	5	2.4	0.1	24.0	15.2	3.3	4.61
40	1	42.2	14.0	3.01	81.9	50.9	1.61
40	3	10.4	2.4	4.33	46.6	15.1	3.09
40	5	3.8	0.5	7.60	26.4	5.8	4.55
50	1	49.2	18.4	2.67	85.6	58.2	1.47
50	3	15.3	3.5	4.37	55.2	20.4	2.71
50	5	6.2	1.1	5.64	34.7	10.0	3.47

FVIII factor VIII, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method

aDoses on Monday and Thursday

bDoses on Monday, Wednesday, and Friday

cRatio of BAY 81-8973:rAHF-PFM

Table 6

Dosing required to maintain FVIII plasma levels >1 IU/dL (simulation of 1000 patients)

Dosing frequency	BAY 81-8973		rAHF-PFM		Ratio^a
Dosing frequency	Dose for 50% of patients to maintain >1 IU/dL, IU/kg	Absolute dose per year for 70-kg patient, IU	Dose for 50% of patients to maintain >1 IU/dL, IU/kg	Absolute dose per year for 70-kg patient, IU	Ratio^a
2×/week	52.4	381,472	161	1,172,080	0.33
3×/week	14.4	157,248	39.1	426,972	0.37

FVIII factor VIII, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method

aRatio of BAY 81-8973:rAHF-PFM

Median time to FVIII threshold level after a single intravenous dose (simulation of 1000 patients) FVIII factor VIII, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method aRatio of BAY 81-8973:rAHF-PFM bDifference of BAY 81-8973 − rAHF-PFM Proportion of patients maintaining FVIII levels above the threshold (simulation of 1000 patients) FVIII factor VIII, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method aDoses on Monday and Thursday bDoses on Monday, Wednesday, and Friday cRatio of BAY 81-8973:rAHF-PFM Dosing required to maintain FVIII plasma levels >1 IU/dL (simulation of 1000 patients) FVIII factor VIII, rAHF-PFM antihemophilic factor (recombinant) plasma/albumin-free method aRatio of BAY 81-8973:rAHF-PFM

Discussion

This open-label, randomized study demonstrated improved PK properties of FVIII with BAY 81-8973 compared with rAHF-PFM following single doses. Mean t ½ was 24% and 16% longer for BAY 81-8973 compared with rAHF-PFM using the one-stage and chromogenic assays, respectively. A prolonged t ½ for BAY 81-8973 versus rAHF-PFM was observed in 16 of 18 patients, indicating that this was a consistent finding. The consistently high degree of sialic acid capping of N-terminal glycans in BAY 81-8973 as a result of a refined manufacturing process [9] may have affected the t ½ of BAY 81-8973, as has been shown for some mammalian proteins [10]. In addition, AUCinf was 32% and 48% higher in patients after infusion with BAY 81-8973 compared with rAHF-PFM using the one-stage and chromogenic assays, respectively. The difference in the PK parameters based on the two assays is not uncommon for FVIII products [9, 15]. In general, the chromogenic assay has higher values for the same sample compared with the one-stage assay, which has been shown for many FVIII products. The popPK models for FVIII after administration of BAY 81-8973 and rAHF-PFM adequately describe the data from this study. The model parameters and results are consistent with a previous popPK analysis [18] and the PK data based on the noncompartmental analysis [9]. The comparison of BAY 81-8973 and rAHF-PFM PK in a single study, as has been done here, is advantageous because across-study comparisons of PK data, including t ½ values, for FVIII products may lead to discrepant and misleading conclusions. For example, reported t ½ for rFVIII-FS ranged from 12.0 to 13.7 h in two published studies and the US prescribing information [9, 19, 20]. In an Octapharma-sponsored study designed to show non-inferiority of simoctocog alfa (Nuwiq®; Octapharma, Stockholm, Sweden) versus rFVIII-FS, t ½ for rFVIII-FS was 16.1 and 18.8 h using the chromogenic and one-stage assays, respectively [14]. For rAHF-PFM, t ½ ranged from 10.4 to 14.7 h across several studies [16, 21–24]. PK variability is influenced by several factors. For example, FVIII CL is highly correlated with von Willebrand factor [25]. Therefore, for an adequate comparison of PK characteristics of FVIII products, the products should be evaluated in the same population of patients. Similar randomized, single-dose, crossover study designs have been used to compare PK parameters between different rFVIII products in other clinical studies. B-domain-deleted rFVIII (BDD-rFVIII) was found to be bioequivalent to rAHF-PFM based on AUC and C max [26]. Turoctocog alfa was also found to be bioequivalent to rAHF-PFM using AUC, C max, incremental recovery, t ½, and CL [27]. In both studies, t ½ was slightly shorter for BDD-rFVIII and turoctocog alfa versus rAHF-PFM [26, 27]. BAY 81-8973 was compared to its predecessor, rFVIII-FS, using a similar trial design; non-inferiority was demonstrated, and AUC and t ½ were increased 19% and 15%, respectively, with BAY 81–8973 versus rFVIII-FS using the chromogenic assay (one-stage assay, 19% and 10% increase for AUC and t ½, respectively, vs. rFVIII-FS) [9]. Although several factors contribute to bleeding phenotype [3], maintenance of FVIII coagulant activity (FVIII:C) levels above threshold levels has been shown to prevent bleeding [8]. Because of the heterogeneity of bleeding phenotype and the high interpatient variability of PK parameters, the optimal threshold level of FVIII:C to prevent bleeding is likely to vary among patients [28, 29]. Nevertheless, FVIII products with favorable PK profiles may increase FVIII:C trough levels to provide additional protection against bleeding [30, 31]. In the current study, simulations using the popPK model, which assumed equivalent efficacy of both products, showed that median time to a trough level of 1 IU/dL FVIII was longer for BAY 81-8973 versus rAHF-PFM, and that a lower dose of BAY 81-8973 compared with rAHF-PFM could achieve a threshold of 1 IU/dL FVIII. Furthermore, because increased trough levels are associated with bleeding protection in some patients [8, 28], increased trough levels for BAY 81-8973 versus rAHF-PFM at the same dose may provide improved bleeding protection with BAY 81-8973. In some patients, prolonged t ½ and higher FVIII levels at various time points may allow for less frequent infusions while still maintaining desired threshold levels. Low annualized bleeding rates were reported in patients randomized to twice-weekly prophylaxis with BAY 81-8973 [12]. Although additional evidence is needed, low annualized bleeding rates may be the result of an improved PK profile for BAY 81-8973 compared with other FVIII products, such as rFVIII-FS [9] and rAHF-PFM (reported in this study). A potential limitation of this study was the need to simulate trough levels at 72 and 96 h because samples were only collected up to 48 h, which is typical for the assessment of PK characteristics of FVIII molecules [9, 26, 27]. However, this potential limitation does not preclude predictions of trough levels at 72 and 96 h because the PK of FVIII molecules are well characterized and the popPK model provided an accurate description of the data.

Conclusions

BAY 81-8973 showed superior PK properties compared with rAHF-PFM following a single infusion in patients with severe hemophilia. Simulations based on popPK modeling showed that a substantially higher proportion of patients could be maintained at trough levels above threshold with BAY 81-8973 compared with rAHF-PFM. A threshold of >1 IU/dL FVIII may be achieved with a lower dose of BAY 81-8973 compared with rAHF-PFM, and median time to 1 IU/dL FVIII was longer for BAY 81-8973 versus rAHF-PFM.

Using a randomized crossover study design in patients with severe hemophilia A, a single infusion of BAY 81-8973 (Kovaltry^®) was associated with significantly improved area under the curve, half-life, mean residence time, and lower clearance compared with a single infusion of antihemophilic factor (recombinant) plasma/albumin-free method (rAHF-PFM [Advate^®]).

Simulation data using a population pharmacokinetic (PK) model indicated that a higher proportion of patients could maintain factor VIII (FVIII) levels above threshold levels of 1, 3, 5, or 10 IU/dL for longer periods of time with BAY 81-8973 compared with rAHF-PFM.

FVIII products with improved PK profiles may provide additional protection against bleeding by increasing FVIII trough levels, and may allow for less frequent infusions in some patients with severe hemophilia A.

27 in total

1. Comparative pharmacokinetics of rVIII-SingleChain and octocog alfa (Advate(®) ) in patients with severe haemophilia A.

Authors: R Klamroth; M Simpson; M von Depka-Prondzinski; J C Gill; M Morfini; J S Powell; E Santagostino; J Davis; A Huth-Kühne; C Leissinger; P Neumeister; D Bensen-Kennedy; A Feussner; T Limsakun; M Zhou; A Veldman; K St Ledger; N Blackman; I Pabinger
Journal: Haemophilia Date: 2016-07-19 Impact factor: 4.287

Review 2. Defining severity of hemophilia: more than factor levels.

Authors: Anna Pavlova; Johannes Oldenburg
Journal: Semin Thromb Hemost Date: 2013-09-11 Impact factor: 4.180

Review 3. Factors that influence the bleeding phenotype in severe hemophilic patients.

Authors: Pablo Rendo; Frank Shafer; Joan M Korth-Bradley; Krupa Sivamurthy; Jorge Korin
Journal: Blood Coagul Fibrinolysis Date: 2013-10 Impact factor: 1.276

4. Population pharmacokinetics of recombinant factor VIII: the relationships of pharmacokinetics to age and body weight.

Authors: Sven Björkman; MyungShin Oh; Gerald Spotts; Phillip Schroth; Sandor Fritsch; Bruce M Ewenstein; Kathleen Casey; Kathelijn Fischer; Victor S Blanchette; Peter W Collins
Journal: Blood Date: 2011-10-31 Impact factor: 22.113

5. Pegylated, full-length, recombinant factor VIII for prophylactic and on-demand treatment of severe hemophilia A.

Authors: Barbara A Konkle; Oleksandra Stasyshyn; Pratima Chowdary; David H Bevan; Tim Mant; Midori Shima; Werner Engl; Jacqueline Dyck-Jones; Monika Fuerlinger; Lisa Patrone; Bruce Ewenstein; Brigitt Abbuehl
Journal: Blood Date: 2015-07-08 Impact factor: 22.113

6. ReFacto and Advate: a single-dose, randomized, two-period crossover pharmacokinetics study in subjects with haemophilia A.

Authors: J Di Paola; M P Smith; R Klamroth; P M Mannucci; C Kollmer; J Feingold; C Kessler; H Pollmann; M Morfini; C Udata; C Rothschild; C Hermans; R Janco
Journal: Haemophilia Date: 2007-03 Impact factor: 4.287

Review 7. Role of enhanced half-life factor VIII and IX in the treatment of haemophilia.

Authors: Ali J Mahdi; Samya G Obaji; Peter W Collins
Journal: Br J Haematol Date: 2015-03-07 Impact factor: 6.998

Review 8. The phenotypic heterogeneity of severe hemophilia.

Authors: Giridhara Rao Jayandharan; Alok Srivastava
Journal: Semin Thromb Hemost Date: 2008-02 Impact factor: 4.180

9. Phase I study of BAY 94-9027, a PEGylated B-domain-deleted recombinant factor VIII with an extended half-life, in subjects with hemophilia A.

Authors: T E Coyle; M T Reding; J C Lin; L A Michaels; A Shah; J Powell
Journal: J Thromb Haemost Date: 2014-04 Impact factor: 5.824

10. Prophylaxis vs. on-demand treatment with BAY 81-8973, a full-length plasma protein-free recombinant factor VIII product: results from a randomized trial (LEOPOLD II).

Authors: K Kavakli; R Yang; L Rusen; H Beckmann; D Tseneklidou-Stoeter; M Maas Enriquez
Journal: J Thromb Haemost Date: 2015-03 Impact factor: 5.824

15 in total

Review 1. BAY 81-8973, a full-length recombinant factor VIII for the treatment of hemophilia A: product review.

Authors: Johnny N Mahlangu; Sanjay P Ahuja; Jerzy Windyga; Nikki Church; Anita Shah; Lawrence Schwartz
Journal: Ther Adv Hematol Date: 2018-06-12

2. Population pharmacokinetic (PopPK) modelling indicates that patients switching to BAY 81-8973 from rFVIII-FS can continue their dosing schedule with improved protection.

Authors: Alexander Solms; Shadan Lalezari; Anita Shah; Gili Kenet
Journal: Haemophilia Date: 2020-04-16 Impact factor: 4.287

3. Increased branching and sialylation of N-linked glycans correlate with an improved pharmacokinetic profile for BAY 81-8973 compared with other full-length rFVIII products.

Authors: John M Teare; David S Kates; Anita Shah; Stephen Garger
Journal: Drug Des Devel Ther Date: 2019-03-22 Impact factor: 4.162

Review 4. Using pharmacokinetics for tailoring prophylaxis in people with hemophilia switching between clotting factor products: A scoping review.

Authors: Jacky K Yu; Alfonso Iorio; Andrea N Edginton
Journal: Res Pract Thromb Haemost Date: 2019-05-20

5. Favorable Pharmacokinetic Characteristics of Extended-Half-Life Recombinant Factor VIII BAY 94-9027 Enable Robust Individual Profiling Using a Population Pharmacokinetic Approach.

Authors: Alexander Solms; Alfonso Iorio; Maurice J Ahsman; Peter Vis; Anita Shah; Erik Berntorp; Dirk Garmann
Journal: Clin Pharmacokinet Date: 2020-05 Impact factor: 6.447

6. Routine clinical care data for population pharmacokinetic modeling: the case for Fanhdi/Alphanate in hemophilia A patients.

Authors: Pierre Chelle; Cindy H T Yeung; Santiago Bonanad; Juan Cristóbal Morales Muñoz; Margareth C Ozelo; Juan Eduardo Megías Vericat; Alfonso Iorio; Jeffrey Spears; Roser Mir; Andrea Edginton
Journal: J Pharmacokinet Pharmacodyn Date: 2019-05-21 Impact factor: 2.745

7. BAY 81-8973 prophylaxis and pharmacokinetics in haemophilia A: Interim results from the TAURUS study.

Authors: Cristina Santoro; Beng Fuh; Phu Quoc Le; Philip Maes; Rubén Berrueco; Eva Maria Mingot-Castellano; Sylvia von Mackensen; Alexander Solms; Michael Wang
Journal: Eur J Haematol Date: 2020-04-23 Impact factor: 2.997

8. BAY 81-8973 demonstrated efficacy, safety and joint status improvement in patients with severe haemophilia A in the LEOPOLD I extension for ≤2 years.

Authors: Johnny Mahlangu; Maria Fernanda Lopez Fernandez; Elena Santagostino; Shadan Lalezari; Despina Tseneklidou-Stoeter; Horst Beckmann; Nikki Church
Journal: Eur J Haematol Date: 2020-03-23 Impact factor: 2.997

9. Relationship between factor VIII activity, bleeds and individual characteristics in severe hemophilia A patients.

Authors: João A Abrantes; Alexander Solms; Dirk Garmann; Elisabet I Nielsen; Siv Jönsson; Mats O Karlsson
Journal: Haematologica Date: 2019-08-01 Impact factor: 9.941

Review 10. Population Pharmacokinetics of Clotting Factor Concentrates and Desmopressin in Hemophilia.

Authors: Tim Preijers; Lisette M Schütte; Marieke J H A Kruip; Marjon H Cnossen; Frank W G Leebeek; Reinier M van Hest; Ron A A Mathôt
Journal: Clin Pharmacokinet Date: 2021-01 Impact factor: 6.447