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

Slides:

Advertisements

Similar presentations

Evaluation of Oral Azacitidine Using Extended Treatment Schedules: A Phase I Study Garcia-Manero G et al. Proc ASH 2010;Abstract 603.

Advertisements

The Reliable Life Defense. Each vial contains: Each vial contains: Recombinant human granulocyte colony-stimulating factor (G-CSF) 300 µg in a volume.

Oncologic Drugs Advisory Committee

AbstractSchema Conclusion Pharmacokinetic profile of the base-excision repair inhibitor Methoxyamine-HCl (TRC102; MX) given as an one-hour intravenous.

Brown JR et al. Proc ASH 2013;Abstract 523.

Scott Butler Infection Innovative Medicines Group AstraZeneca R&D, Boston CPTR Workshop, 2012 Arlington, VA AZD5847 Oxazolidinone for the treatment of.

Response Optimization in Oncology In Vivo Studies: a Multiobjective Modeling Approach Maksim Pashkevich, PhD (Early Phase Oncology Statistics) Joint work.

Introduction to PKPD Modelling – Applications Joe Standing June 2012 UCL Institute of Child Health & Great Ormond Street Hospital for Children, London.

Roberts AW et al. Proc ASH 2014;Abstract 325.

Title, in bold style Subtitle, in regular Max 3 lines of text totally NB! The graphic outside the slide will not show in “Slide Show” or on print WntResearch.

Cancer Nanotechnology: New Opportunities for Targeted Therapies FDA Public Meeting October 10, 2006 Piotr Grodzinski, Ph.D. Director, Nanotechnology for.

Office of Clinical Pharmacology and Biopharmaceutics IDSA/ISAP/FDA Workshop 4/16/04 1 Improvement in Dose Selection: FDA Perspective IDSA/ISAP/FDA Workshop.

Phase III Randomized, Placebo-Controlled, Double-Blind Study of Intravenous Calcium/Magnesium to Prevent Oxaliplatin- Induced Sensory Neurotoxicity, N08CB.

1 Phase II trial of sequential gemcitabine and carboplatin followed by paclitaxel as first-line treatment of advanced urothelial carcinoma Presented by.

1 Clinical PK Optimal design and QT-prolongation detection in oncology studies Sylvain Fouliard & Marylore Chenel Department of clinical PK, Institut de.

Comparison of Nilotinib and Imatinib in Patients with Newly Diagnosed Chronic Myeloid Leukemia in Chronic Phase (CML-CP): ENESTnd Beyond One Year Larson.

Taxane-pretreated metastatic breast cancer (MBC): investigational agents TTP = median time to disease progression OS = median overall survival.

Frontline Therapy with Brentuximab Vedotin Combined with ABVD or AVD in Patients with Newly Diagnosed Advanced Stage Hodgkin Lymphoma Younes A et al. Proc.

Phase 1 Clinical Studies First-In-Human (FIH) Pharmacologically-Guided Dose Escalation Jerry M. Collins, Ph.D. Developmental Therapeutics Program Division.

Thymidine phosphorylase (TP) upregulation Dose- and time-dependent upregulation of TP in human colon cancer xenografts PaclitaxelDocetaxel.

Results: In the presence of PD measurements, PK data provided little additional information. By a limited PD sampling the number of patients on target.

Anthe Zandvliet, Anton de Haan, Pieta IJzerman-Boon, Rik de Greef, Thomas Kerbusch PAGE meeting 2008 PK-PD model of multiple follicular development during.

APPLYING PRE-CLINICAL DATA TO CLINICAL STUDIES-I Edward A. Sausville, M.D., Ph.D. Developmental Therapeutics Program National Cancer Institute October.

Predictive Models of Cancer Xenograft Models Of Childhood Solid Tumors Solid Malignancies Group St. Jude Children’s Research Hospital.

Modeling of Longitudinal Tumor Size Data in Clinical Oncology Studies of Drugs in Combination N. Frances 1, L. Claret 2, F. Schaedeli Stark 3, R. Bruno.

Predicting toxicity for patients with advanced Gastrointestinal Stromal Tumors (GIST) treated with imatinib mesylate : an EORTC/ISG/AGITG randomized trial.

EMEA London Pharmacokinetic- pharmacodynamic integration in veterinary drug development: an overview P.L. Toutain National Veterinary School ;Toulouse.

Phase III trial of chemotherapy with or without irinotecan in the front-line treatment of metastatic colorectal cancer in elderly patients. FFCD

Objective: To utilize preclinical and phase I PK/PD data from a new quinolone (Q) and relevant public domain data to develop an exposure-response model.

Taiwan 2000 Comparative evaluation in tolerance of neoadjuvant versus adjuvant docetaxel based chemotherapy in resectable gastric cancer in a randomized.

Conclusions An appreciable dose-concentration-response relationship between NN1731 and F 1+2 was expressed in a population PK/PD model. Since F 1+2 appearance.

The New Drug Development Process (www. fda. gov/cder/handbook/develop

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

Updated Results of a Phase I First-in-Human Study of the BCL-2 Inhibitor ABT-199 (GDC-0199) in Patients with Relapsed/Refractory (R/R) Chronic Lymphocytic.

AN EXAMPLE OF APPLICATION OF THE POPULATION APPROACH TO TOXICOLOGICAL STUDIES F. Fiorentini 1, M. Simeoni 2, I. Poggesi 1, G. Westerberg 1, M. Rocchetti.

Model-based dose selection for next dose- finding trial 1. Introduction Exploratory clinical development trials often include biomarkers or clinical readout.

Inotuzumab Ozogamicin (IO; CMC544), a CD22 Monoclonal Antibody Attached to Calicheamycin, Produces Complete Response (CR) plus Complete Marrow Response.

TAXOL® (paclitaxel) for Adjuvant Treatment of Node Positive Breast Cancer Oncologic Drugs Advisory Committee TAXOL® (paclitaxel) for Adjuvant Treatment.

Cooperative Clinical Trials with 13-Cis-Retinoic Acid in Neuroblastoma Katherine K. Matthay, M.D University of California, San Francisco Children’s Oncology.

12 th Annual CTOS Meeting 2006 AP23573 Induced Long-term Stability in 2 Patients with Desmoplastic Small Round Cell Tumor (#561) Scott Schuetze, Warren.

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

Ibrutinib in Combination with Rituximab (iR) Is Well Tolerated and Induces a High Rate of Durable Remissions in Patients with High- Risk Chronic Lymphocytic.

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

Copyright © 2008 Merck & Co., Inc., Whitehouse Station, New Jersey, USA All rights Reserved Pharmacokinetic/Pharmacodynamic (PK/PD) Analyses for Raltegravir.

| 1 Application of a Bayesian strategy for monitoring multiple outcomes in early oncology clinical trials Application of a Bayesian strategy for monitoring.

Kantarjian HM et al. Proc ASH 2012;Abstract Long-Term Follow-Up of Ongoing Patients in 2 Studies of Omacetaxine Mepesuccinate for Chronic Myeloid.

The process of drug development. Drug development 0,8 – 1 mld. USD.

Confidential and Proprietary Business Information. For Internal Use Only. Statistical modeling of tumor regrowth experiment in xenograft studies May 18.

Lung Cancer Cell Line Nº StudiesStrainNº Mice H44113Athymic nude119 A5492CB-17scid15 Calu-62CD-1 nu/nu25 H16501Athymic nude8 H19751Athymic nude8 H21226Athymic.

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

The Stages of a Clinical Trial

CCO Independent Conference Coverage

PHASE I/II STUDY OF PEGYLATED LIPOSOMAL DOXORUCIN (PLD) AND GEMCITABINE (GEM) IN RECURRENT PLATIN RESISTANT OVARIAN CANCER (OC). A Study of the VWOG.

Use of Physiologically Based Pharmacokinetic (PBPK) Models to Support Canine Drug Product Development Devendra Pade1, Marilyn Martinez2, Bipin Mistry2.

Multiple Model Dosage Design

Telephone    Provider of Global Contract Research Services Accelerating Preclinical Research, Drug Discovery.

Background and Objectives

RAT SIMULATION RESULTS HUMAN SIMULATION RESULTS

Krop I et al. SABCS 2009;Abstract 5090.

Nat. Rev. Clin. Oncol. doi: /nrclinonc

Longitudinal Analysis Beyond effect size

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

Seymour JF et al. Proc ASH 2013;Abstract 872.

Injury of primary afferent neurons may contribute to osteoarthritis induced pain: an experimental study using the collagenase model in rats S. Adães,

Pollyea DA et al. Proc ASCO 2011;Abstract 6505.

Ahmadi T et al. Proc ASH 2011;Abstract 266.

Telephone    Provider of Global Contract Research Services Accelerating Preclinical Research, Drug Discovery.

Yang Liu, Anne Chain, Rebecca Wrishko,

role of comparative oncology in translational research

Telephone    Provider of Global Contract Research Services Accelerating Preclinical Research, Drug Discovery.

Presentation transcript:

Background Objectives Data Simulation in human Conclusion -F14512, a polyamine-vectorized anti-cancer drug which combines an epipodophyllotoxin core targeting topoisomerase II with a spermine moiety as a tumor cell-delivery vector [1]. -Currently in clinical phase II study in combination with aracytine for patients with acute myeloid leukemia, F14512 was also investigated in ovarian cancer patients. -In parallel, F14512 is tested in pet dogs with naturally occuring lymphoma [2]. [1] Barret JM et al. Cancer Res Dec 1;68(23): [2] Tierny F et al. Submitted in Clinical Cancer Research- Under review. [3] Friberg LE et al Dec;28(6): [4] Friberg LE et al 2002 Dec 15;20(24): References The aim of the present study was to retrospectively assess the human predictability of semi-physiological leukopenia PK/PD models built on rats, Beagle laboratory dogs and pet dogs. Model building A same semi-physiological PK/PD model of leukopenia was used to fit the data of the 3 groups of animals (rat, beagle dogs and pet dogs) separately. [3] Estimate (RSE %) RatBeagle dogPet Dogs Typical values WBC 0 (x 10 9 /L) 14.8 (2 %)7.51 (3 %)10.9 (9 %) MTT (h) 74.7 (10 %)77.1 (4 %)63.6 (6 %) γ FIX [4] 0.2 FIX0.15 (13 %) Slope (L/mg) 5.12 (7%)59.3 (10 %)48.1 (14 %) Inter individual variabilities, CV (%) WBC % (21%)15.5 % (58 %)32 % (28 %) MTT % (57 %) Slope % (33 %) Residual variability, CV% Prop. PD error 18.1 % (10%)25.2 % (20%)44.2 % (12 %) Models Estimated Slope from Animal (L/mg) fu human / fu animal Fu corrected predicted Slope in human (L/mg) IC90 animal /IC90 human Fu and sensivity corrected predicted Slope in human (L/mg) Rat Beagle dog Pet dog Human Protein binding study in vitro stem cells study Simulation with rat slope Simulation with Beagle dog slope Simulation with Pet dog slope - Actual myelosuppression in human was considerably under-estimated by the rat model - Both Pet / Beagle dogs models with fu correction provided a good prediction of human leukopenia induced by F Considering correction for inter species differences in bone marrow sensitivity would have resulted in a large under-prediction of the human myelosuppression - PK/PD models based on larger species such as pet dogs may be a useful translational tool and its application in better predicting hematotoxicity in FIH trials can be valuable. 5 mg/m 2 /QD for 3 days 10 mg/m 2 /QD for 3 days Median of simulations Median of observations P5, P95 of simulations Observed data VPC - Rat model RatsBeagle dogsPet dogs Studies1 PK/PD3 toxicity1 clinical Schedule QD : once a day ; BID : twice daily ; SD : single dose SDQDBID SD and repeated doses (2/weeks) QD for 3 days every 2 weeks Administration routeiv bolus iv infusion (3h) Doses (mg/kg)1; 2; 30.4 ; 0.7 From 0.03 to 0.85From 0.05 to Number of animals Number of observations Ratio of unbound fraction human / animal Ratio of IC90 animal/human * Observed WBC counts in 11 patients included in a phase I ovarian cancer study where F14512 was administered as a 3h infusion once daily for 3 days System (physiological) parameters : - MTT = 4/ktr (Kprol=kcirc=ktr) - WBC 0 =baseline of WBC - γ=Feed back Drug dependant parameter : - Slope Structure of the PK-PD model describing chemotherapy induced myelosuppression Simulations were performed considering - data from the 11 patients included in the ovarian cancer study: -Individual baseline values of WBC -Individual PK parameters (EBE obtained with the post hoc options) -System related parameters of the PK/PD models previously established: -MTT=125 h (IIV,CV=26 %) and γ=0.17 [4] -Slopes estimated with PK/PD modeling in animals (IIV,CV=45%) and adjusted with the unbound fraction but without considering the inter-species in vitro sensivity results * Results of an in vitro evaluation of F14512 haematotoxicity on CFU-GM hematopoietic progenitor VPC – Beagle dog modelVPC – Pet dog model PK/PD sequential strategy :  Population PK parameters for rat and beagle dogs models  Individual PK parameters for Pet Dog model Nonmem 7.2 FOCE method Log transformed data SD Doses : 0.1 and 0.35 mg/kg 2 / week Doses : 0.03; 0.1; 0.35 Admin days : 1–5– Doses : mg/kg Admin days : 1–5–15 Dose 0.5 mg/kg Prediction interval of simulations in black Observed values in blue Inter-species comparison of semi-physiological pre-clinical PK/PD models to better predict the time course of myelosuppression in human: application to a novel vectorized epipodophyllotoxin (F14512) A. Petain (1), B. Gomes (1), D. Tierny (2), A. Bidaut (1), P. Ferre (1) and L. Nguyen (1) (1) Institut de Recherche Pierre Fabre, Research & Development center, Toulouse, France (2) Oncovet Clinical research, Villeneuve d’Ascq, France