The aim of this study was to characterise the population pharmacokinetics of tacrolimus in paediatric SCT recipients in the first year post-transplant;

Slides:

Advertisements

Similar presentations

Karunya Kandimalla, Ph.D

Advertisements

PHARMACOKINETIC MODELS

OPTN Modifications to Heart Allocation Policy Implemented July 12, 2006 Changed the allocation order for medically urgent (Status 1A and 1B) patients Policy.

Instant Clinical Pharmacology E.J. Begg

First, zero, pseudo-zero order elimination Clearance

Clinical Pharmacokinetics

POPULATION PHARMACOKINETICS OF CEFTRIAXONE IN INTENSIVE CARE UNIT (ICU) ADULT PATIENTS C Le Guellec (1), N Simon (2), D.Garot (3), R. Respaud (1), P Lanotte.

Preventing Medication Errors in Pediatric and Neonatal Patients

1 Rash and Low T2* MRI in a Paediatric Thalassaemia Patient.

Pharmacokinetics as a Tool

Background and Objectives Methods and Materials Results Conclusions References Increased computing power gives us the possibility of building more complex.

Effect of Obesity on Kidney Transplantation Reference: Potluri K, Hou S. Obesity in kidney transplant recipients and candidates. Am J Kidney Dis. 2010;56:143–156.

Nonlinear pharmacokinetics

Laplace transformation

Basis for Neulasta® (Pegfilgrastim) Approval

Copyright © 2013, 2010 by Saunders, an imprint of Elsevier Inc. Chapter 10 Drug Therapy in Pediatric Patients.

Figure 1. Diagnostic plots for propofol pharmacokinetics and effect (BIS) in morbidly obese patients including observations versus individual- predictions.

Dose Prediction of Tacrolimus in de novo Kidney Transplant Patients with Population Pharmacokinetic Modelling Including Genetic Polymorphisms. R.R. Press.

INTRAVENOUS INFUSION.

Modelling and Simulation Group, School of Pharmacy Pharmacokinetic design optimization in children and estimation of maturation parameters: example of.

Figure 2. The efficiency with the different optimizations compared to the standard design. 100 % effeciency indicates no improvement compared to the standard.

PK/PD Modeling in Support of Drug Development Alan Hartford, Ph.D. Associate Director Scientific Staff Clinical Pharmacology Statistics Merck Research.

Valproic Acid Software and Presentation by: Ted, Rob, Jeff, Cassie, Tristan, Korin, Ron, Gabe, Matt, Judith, Lindsay.

© 2010 Universitair Ziekenhuis Gent Population pharmacokinetics of tacrolimus in stable paediatric renal transplant recipients translated into clinical.

Animal Studies and Human Health Consequences Sorell L. Schwartz, Ph.D. Department of Pharmacology Georgetown University Medical Center.

Background Objectives Data Simulation in human Conclusion -F14512, a polyamine-vectorized anti-cancer drug which combines an epipodophyllotoxin core targeting.

Results: Accuracy and precision expressed as MPE and RMSE was better for the proposed model compared to the Sam and Staatz models. Graphical diagnostics.

FDA Case Studies Pediatric Oncology Subcommittee March 4, 2003.

Population Pharmacokinetic Characteristics of Levosulpiride and Terbinafine in Healthy Male Korean Volunteers Yong-Bok Lee College of Pharmacy and Institute.

APPLICATION OF INDIVIDUALIZED BAYESIAN UREA KINETIC MODELING TO PEDIATRIC HEMODIALYSIS Olivera Marsenic, Athena Zuppa, Jeffrey S. Barrett, Marc Pfister.

Drug Administration Pharmacokinetic Phase (Time course of ADME processes) Absorption Distribution Pharmaceutical Phase Disintegration of the Dosage Form.

Rivaroxaban Has Predictable Pharmacokinetics (PK) and Pharmacodynamics (PD) When Given Once or Twice Daily for the Treatment of Acute, Proximal Deep Vein.

Continuous intravenous infusion (one-compartment model)

Modelling and Simulation Lab, School of Pharmacy, University of Otago, New Zealand D-optimal Adaptive Bridging Studies in Pharmacokinetics Lee-Kien Foo.

Prof. Dr. Henny Lucida, Apt

Background Conclusions low weight, CYP3A5*1 allele, low gamma glutamyl transpeptidase and low hematocrit are associated with a higher tacrolimus clearance.

Pharmacokinetics of Vancomycin in Adult Oncology Patients Hadeel Al-Kofide MS.c; Iman Zaghloul PhD; and Lamya Al-Naim PharmD Department of Clinical Pharmacy,

INTERMITTENT IV VANCOMYCIN WHAT DOSE SHOULD WE START WITH?

Design of Sustained Release Dosage Forms

1.Andersson, T, et al. Clin Pharmacokinet 2001;40: Hassan-Alin, M, et al. Eur J Clin Pharmacol 2000;56: Population Pharmacokinetic Modelling.

1. Objectives Novartis is developing a new triple fixed-dose combination product. As part of the clinical pharmacology program, pharmacokinetic (PK) drug-drug.

Foundation Knowledge and Skills

Pharmacokinetics (PK) and Pharmacodynamics (PD) of Rivaroxaban: A Comparison of Once- and Twice-daily Dosing in Patients Undergoing Total Hip Replacement.

HAPLOIDENTICAL STEM CELL TRANSPLANT

Pharmacokinetics 3rd Lecture

Compartmental Models and Volume of Distribution

Population pharmacokinetic-pharmacodynamic modeling of furosemide for anti-hypertensive effect Mahendra Shukla1,2 , Moon Jain2,3, Swati Jaiswal1,2 , Abhisheak.

Fig. 1. CsA blood concentration time curve according to the population model (dashed line), the actual measured CsA blood concentrations at t=0, 2 and.

RAXIBACUMAB DB08902 C6320H9794N1702O1998S kDa CATEGORY

Chapter 9 PHARMACOKINETICS VARIABILITY

Pharmacokinetics of Vancomycin in Adult Oncology Patients

Using extrapolation to support a pediatric investigational plan: an application in liver transplantation development Thomas Dumortier, Martin Fink, Ovidiu.

Anticonvulsants: Valproic acid

Quantitative Pharmacokinetics

Variable Eculizumab Clearance Requires Pharmacodynamic Monitoring to Optimize Therapy for Thrombotic Microangiopathy after Hematopoietic Stem Cell Transplantation

Shahad Abbas1,2 Alison H Thomson1,2 B) non-malignant patients.

Background and Objectives

Clinical Pharmacokinetics

Clinical Pharmacokinetics

Variable Eculizumab Clearance Requires Pharmacodynamic Monitoring to Optimize Therapy for Thrombotic Microangiopathy after Hematopoietic Stem Cell Transplantation

Safety, Pharmacokinetics, and Efficacy of Palifermin in Children and Adolescents with Acute Leukemias Undergoing Myeloablative Therapy and Allogeneic.

Predictive Performance of a Myelosuppression Model for Dose Individualization; Impact of Type and Amount of Information Provided Johan E. Wallin, Lena.

Developmental pharmacokinetics of morphine and its metabolites in neonates, infants and young children N.J. Bouwmeester, B.J. Anderson, D Tibboel, N.H.G.

Onset of thymic recovery and plateau of thymic output are differentially regulated after stem cell transplantation in children Matthias Eyrich, Gernot.

Selected Bioavailability and Pharmacokinetic Calculations

1 Concentration-time curve

High-Dose Weekly AmBisome Antifungal Prophylaxis in Pediatric Patients Undergoing Hematopoietic Stem Cell Transplantation: A Pharmacokinetic Study Parinda.

REFERENCE: APPLIED CLINICAL Slideshow by: lecturer HADEEL DELMAN

Eculizumab Therapy in Children with Severe Hematopoietic Stem Cell Transplantation– Associated Thrombotic Microangiopathy Sonata Jodele, Tsuyoshi Fukuda,

Presentation transcript:

The aim of this study was to characterise the population pharmacokinetics of tacrolimus in paediatric SCT recipients in the first year post-transplant; to identify factors that may explain pharmacokinetic variability; and to develop an Excel-based dosing macro, utilising the model and Bayesian forecasting techniques, to assist with tacrolimus dosing in new paediatric SCT recipients. All subjects received tacrolimus initially as a continuous intravenous infusion at 0.03 mg/kg/day, starting two days before transplantation. Patients were converted to oral tacrolimus therapy two to three weeks after transplantation, divided into twice daily administration. A one-compartment model with first order absorption and elimination was considered sufficient to describe the data. In the final model, mean CL was L/h/kg 0.75, V was 8.97 L/kg and bioavailability (F) was 12.5% (Tab.1). Inter-individual variability in CL, V and F was 57%, 104% and 61%, respectively. Covariate analysis suggested tacrolimus CL positively correlated with CrCL. Typical value of CL varied from L/h/kg 0.75 at the minimum and maximum CrCL values. Population Pharmacokinetics of Tacrolimus in Paediatric Haematopoietic Stem Cell Transplantation and Implementation in a Dose Adaptation Tool Johan E. Wallin 1, Lena E. Friberg 1, Anders Fasth 2 and Christine E. Staatz 3 1. Div. Pharmacokinetics & Drug Therapy, Uppsala University, Sweden 2. Dept.Pediatrics, University of Gothenburg, Gothenburg, Sweden 3. School of Pharmacy, University of Queensland, Brisbane, Australia. Tacrolimus is a valuable immunosuppressant option to ciclosporin in the prevention of graft-versus-host disease (GVHD) following allogeneic hematopoietic stem cell transplantation (SCT). Limited data is available on the pharmacokinetics of tacrolimus in paediatric hematopoietic stem cell recipients. Data were collected retrospectively from the medical records of 22 children transplanted between 1997 and 2007 at the Queen Silvia’s Children’s Hospital in Gothenburg, Sweden. Population pharmacokinetic analysis was performed using NONMEM version 6. Tacrolimus distribution volume (V) and clearance (CL) were allometrically scaled to lean body weight. A previously suggested model with a time-dependent increase in tacrolimus apparent clearance (CL/F) developed for liver transplant patients [1] was compared to a simpler one- and two- compartment model. A step-wise covariate search was performed where covariates screened for influence on the pharmacokinetic parameters were liver function tests (AST, ALT, GGT, ALP), bilirubin, albumin, creatinine clearance (Schwartz formula), sex, age and post-operative day (POD). Background Results and Discussion F decreased with time post-transplant, to only 4.5% after a year. The estimated bioavailability was approximately half that reported in adult SCT recipients, whereas CL and V values were similar to adult values [2]. A time dependent error model was chosen, where the error component decline during the first days of therapy. Model goodness of fit plots can be seen in Fig.1. A macro was constructed in MS Excel to select an initial tacrolimus dose based on the final covariate model (Fig.2). Measured drug concentration can be used in a Bayesian function to estimate individual parameters for dose adaptation to maximize the likelihood of achieving target concentrations at the time of transplantation. The population model indicated the need for a 50% higher initial dose than the current for the typical individual to achieve the target concentration at the time of transplantation, alternatively starting the treatment 24 hours earlier. Table 1. Final model parameters Routine therapeutic drug monitoring can be implemented in our dosage adaptation tool to assist with tacrolimus dosing in new paediatric SCT recipients. In future work, sample times for maximum information on an individual level will be evaluated using optimal design analysis. Methods Aim Conclusion References 1.Antignac, M., et al., Population pharmacokinetics of tacrolimus in full liver transplant patients: modelling of the post-operative clearance. Eur J Clin Pharmacol, (5-6): p Jacobson, P., et al., Factors affecting the pharmacokinetics of tacrolimus (FK506) in hematopoietic cell transplant (HCT) patients. Bone Marrow Transplant, (8): p Figure 2. Macro with covariate guided initial dose and Bayesian adaptation to achieve the target concentration (12-15 ng/ml) Typical valueRSE Inter individual variability RSE CL0.124 L//h/kg %57%28% CL – CrCL % V8.97 L/kg20%104%37%5 F12.5%1261%33% F-POD % Prop. error %18%62% Time dep. prop.error % Half life time dep. Error2.3 days44% Figure 1. Goodness of fit-plots for the final model log