ADMET : Pharmaceuticals : All

Conference Overview

ADMET screening is crucial to the drug development process and assists the elimination rate of weak drug candidates early in the drug-discovery process, and decreases the proportion of compounds failing in clinical trials for ADMET reasons. SAE Media Group's 5^th Annual ADMET Conference will bring you up to date with the latest developments, technologies and techniques that are in use across the industry and look towards the future.

By attending this conference, you will learn:

How to effectively integrate ADMET optimisation into drug discovery to reduce attrition rates from AstraZeneca
Strategies for predicting drug-drug interactions arising from CYP450 inhibition from Pfizer
How to develop a mechanism-based PK/PD model from Eli Lilly
The application of High Content Analysis for predictive cytotoxicity testing & preclinical toxicity biomarkers from University College Dublin
Tools and strategies to consider in characterising and investigating hepatotoxicity from Genetech
What the emerging in vitro toxicity assays are and the role of stem cells in assessing human toxicology from Roche
Case studies demonstrating the benefits of evaluating PK in early stage drug development from Merck

The conference will provide a look at how the big names in the pharma industry are approaching ADMET. With a case study focus and presentations from companies including Novartis, AstraZeneca, Pfizer, Eli Lilly, Genentech, MSD, Merck & Co., Roche, Gedeon Richter and more along with distinguished representatives from top academic organisations this conference promises to provide an intimate environment for benchmarking against industry leaders and networking.

Featured Presentations:

Building hypotheses in lead selection and optimisation
Bernard Faller, Director of Metabolism & Pharmacokinetics / in-vitro ADME, Novartis, Switzerland
ADME Optimisation in Early- and Late-Phase Drug Discovery
Gerhard Gross, Global Discipline Leader ADME, AstraZeneca, UK
In Vitro and In Vivo Approaches for Assessing the Potential for Drug Induced Liver Injury
Donna Dambach, Director, Investigative Safety Assessment, Genentech, USA
Emerging In Vitro Toxicity Assays and the Role of Stem Cells in Assessing Human Toxicology
Claudia McGinnis, Group Head, In Vitro Toxicology, Roche, Switzerland

For speaker opportunities, contact SAE Media Groupproduction@SAE Media Group-online.co.uk

For sponsorship and exhibitioning opportunities, contact sponsorshipdept@SAE Media Group-online.co.uk

Bernard Faller
Director of Metabolism & Pharmacokinetics / in-vitro ADME
Novartis

Donna Dambach
Director, Investigative Safety Assessment
Genentech

Gerhard Gross
Global Discipline Leader ADME
AstraZeneca

Claudia McGinnis
Group Head, In Vitro Toxicology
Roche

Willem Schoonen
Senior Research Scientist, Toxicology & Drug Disposition
MSD

Punam Sandhu
Senior Investigator
Merck

Kuresh Youdim
Senior Principal Scientist
Pfizer

Richard Weaver
Associate Principal Scientist
AstraZeneca

See the full lineup...

Conference agenda

Day one
Day two

8:30

Registration & Coffee
9:00

Chairman's Opening Remarks
Bernard Faller, Director of Metabolism & Pharmacokinetics / in-vitro ADME, Novartis Pharmaceuticals
9:05

ADME Optimisation in Early- and Late-Phase Drug Discovery
Gerhard Gross, Global Discipline Leader ADME, AstraZeneca

Applicability domain and validity

Decision points

Preclinical strategies

False positive rates

9:35

Targeting Drugs for the Brain
Hinnerk Boriss, CEO, Sovicell

Fast and reliable prediction of brain disposition and free drug available in brain

Classification of CNS versus non-CNS drugs based on rate and extent

Prediction of CNS side-effects

10:15

Morning Coffee
10:45

Probabilistic Model of Regioselectivity of Metabolism in Human Liver Microsomes
Pranas Japertas, Director of ADMET and PhysChem, Advanced Chemistry Development Labs

A ligand-based model of regioselectivity, based on >850 structures

Predicting probability to be a metabolism site for every atom in the molecule using separate models for different reactions

Estimation of the reliability of prediction defining the model applicability domain

Possibility to expand this applicability domain using in-house data

11:25

Vinblastine Treated CaCo-2 Culture as a Drug Penetration Model
Monika Vastag, Head of In vitro Metabolism Laboratory, Gedeon Richter

Characterisation of efflux transporters: function and importance

Experimental approaches to identify P-gp substrates/inhibitors

Comparison of cell culture models of drug penetration

Establishment and characterisation of vinblastine treated Caco-2 culture

Validation of the vinblastine treated Caco-2 penetration assay

Practice of penetrability screening of new chemical entities in our preclinical research

11:55

Integrating Predictive ADMET into Hit to Lead and Optimisation
Robert Clark, Director of Life Sciences, Simulations Plus

Hedging your bets by including ADMET diversity dimensions

Balancing potential ADMET liability against potential potency, selectivity etc.

Accommodating the inherent fuzziness of ADMET exclusion thresholds

Managing interdependence among biological and physical properties

12:35

Networking Lunch
13:35

Structure-based ADMET Studies
Frank Blaney, Director, MemProt Consulting

Metabolite prediction of CypP450 reactions

Toxicity from Nuclear Receptors

Understanding P-glycoprotein interactions

Efforts towards predicting hERG liability

14:05

RAPIDD plus
Helen McKeever, Programme Manager, Almac Group

Addressing challenges of increasing time-to-market, cost and attrition

Integrated drug and biomarker development in a pre-clinical setting

14:45

Building Hypotheses in Lead Selection and Optimisation
Bernard Faller, Director of Metabolism & Pharmacokinetics / in-vitro ADME, Novartis Pharmaceuticals

Translating PK parameters into MedChem actions

When can one use rules derived from the analysis of generic drugs?

Extracting information from the absence of correlation

15:15

Afternoon Tea
15:45

Supersaturation Effects in Solubility-Enhancing Excipients and Biorelevant Media
John Comer, Co-founder & Technical Director, Sirius Analytical Instruments
16:20

Prediction of DDI's Arising from Cytochrome P450 Inhibition
Kuresh Youdim, Senior Principal Scientist, Pfizer

Importance of understanding CYP inhibition

Extrapolation of in vitro data to predict clinical interactions following CYP inhibition

Factors influencing the extent of a DDI due to CYP inhibition

Future Directions

16:50

Developing a Mechanism-based PK/PD Model
Damien Cronier, Research Scientist, Global PK/PD, Eli Lilly

Influencing early phase development using preclinical models

Connecting the PK with the pharmacology and pre-clinical efficacy of the compound

Providing an improved rationale for selecting the dose rage for Phase I trials

17:20

Drug Transporter Assays in Discovery
Laurent Salphati, Scientist, Genentech

Available assays

How assays are used in the screening cascades

Utilization of the data (case study)

17:50

Chairman’s Closing Remarks and Close of Day One
8:30

Registration & Coffee
9:00

Chairman's Opening Remarks
Donna Dambach, Director, Investigative Safety Assessment, Genentech
9:10

The Utility and Application of TDI Screens in Early Discovery DMPK
Richard Weaver, Associate Principal Scientist, AstraZeneca

Importance of front-loading TDI assays in Discovery

In vitro - in vivo DDI extrapolation

MBI data as a Reactive Metabolite early-warning flag

9:45

System-dependent inhibition of cytochrome P450 (CYP) enzymes
Andrew Parkinson, Chief Scientific Officer, XenoTech

When should cytochrome P450 (CYP) inhibition by drug candidates be evaluated in human hepatocytes and not just human liver microsomes or recombinant CYP enzymes?

Rules to guide the selection of the appropriate test system to evaluate CYP inhibition

Common errors associated with the processing of data from metabolism-dependent inhibition (MDI) studies that incorporate a dilution step.

Why a dilution step - even with correct data processing - should be avoided in evaluating drug candidates MDI of CYP enzymes

10:25

Morning Coffee
10:55

Integrating Predictive Toxicology Model Development

Data Management, Schema and Integrating Multiple Resources

Predictive Toxicology Application-oriented Ontology Development

Developing combined in silico in vitro Consensus Models

Model Validation and Applicability Domain

Incorporating Pharmacokinetics to Predict Exposure

OpenTox Case Study Example

Barry Hardy, Director, Community of Practice & Research Activities and OpenTox Project Coordinator, Douglas Connect
Nina Jeliazkova, Technology Director and OpenTox Lead Developer, Ideaconsult
11:40

Application of High Content Analysis for Predictive Cytotoxicity Testing & Preclinical Toxicity Biomarkers
View Bio

Peter O'Brien, Veterinary Clinical Pathologist / Toxicologist, University College Dublin
After Peter's DVM training in Saskatchewan, he obtained his PhD in Veterinary Physiology and Pharmacology in Minnesota, then his board certification in Veterinary Clinical Pathology in Guelph, where he served on faculty for 7 years. Peter was recruited into drug safety evaluation in 1995, first to Procter & Gamble in Cincinnati Ohio, then in 1997 to SmithKline Beecham - UK, and in 2001 to Pfizer at Sandwich. His experience has been in developing and managing state-of-the-art Clinical Pathology labs that provide biomarkers for Discovery and Pre-Clinical Development. At Pfizer, Peter headed Discovery Toxicology Biomarkers labs for Safety Sciences – Europe and developed and validated mechanistic safety biomarkers to enhance preclinical confidence in safety, reduce attrition of drug candidates, and for use in preclinical and clinical monitoring. In late 2006 Peter returned to academia where he continues his work on translational safety biomarkers at University College Dublin. Here, in 2008 Peter established Advanced Diagnostics Laboratories, Ltd as a commercial spin-off lab to provide toxicology biomarkers service.

Criteria for effective cytotoxicity models

Demonstration of predictive cytotoxicity screens and investigations of toxicity mechanisms

Demonstration of toxicity in vivo using high content analysis of peripheral blood lymphocytes

Application strategies for screening for toxicity, identification of mechanisms, and development of translational in vivo biomarkers of toxicity

12:15

Segregation of Genotoxic Compounds
Willem Schoonen, Senior Research Scientist, Toxicology & Drug Disposition, MSD

Genotoxicity testing in the early phase of the drug development process

Segregation of Genotoxicity scores from Salmonella, Yeast and HepG2 cells

HepG2 cells
- analysis with toxicogenomics for global gene expression profiling of genotoxicants
- validation of promoter based luciferase reporter assays with the promoters of RAD51C, and Cystatin A, and the responsive elements of p53 and Nrf2
- in vitro micronuclei analysis with high content screening, the more traditional way
- advantage of endogenous metabolism by phase I and II enzymes

12:50

Networking Lunch
13:50

In Vitro and In Vivo Approaches for Assessing the Potential for Drug Induced Liver Injury
Donna Dambach, Director, Investigative Safety Assessment, Genentech

The line between overt toxicity, "outliers" and idiosyncratic toxicity

In vitro-in vivo correlations-consideration of physiochemical and PK drivers of toxicity

Assessing metabolism as the basis for toxicity

Preclinical genomic assessments and their potential clinical application

Clinical trial sampling-leveraging new, 'standard' endpoints

14:25

Emerging In Vitro Toxicity Assays and the Role of Stem Cells in Assessing Human Toxicology
Stephan Kirchner, Lab Head, In vitro Screening, F. Hoffmann-La Roche

Microscale cell culture systems: novel approaches that mimic regulatory tests and allow for higher-throughput testing

Current status of the development of human embryonic stem cell-derived tissue-specific cells and their applications

15:00

Mechanisms of Human (Hepato)Toxicity
Katya Tsaioun, President, Apredica

Business and science arguments for and against early investigation of mechanisms of toxicity

Known mechanisms of human hepatotoxicity

Assays available for prediction of specific mechanisms of toxicity:

HCA, mitochondrial toxicity, phospholipidosis: validation

Case studies: when and which assays are relevant?

Path forward: new cell and tissue models

15:40

Afternoon Tea
16:10

Metabolism-Based Drug Toxicity in Drug Development
Timothy Schulz-Utermoehl, Group Manager, In Vitro ADME, Clinical Pharmacology & DMPK, AstraZeneca

Case Study 1 - Assessing the value of reactive metabolite assays

Looking to past failures - could we have predicted toxicity using modern in vitro tools?

Determining the cause(s) of species differentiation in toxicity

Case Study 2 - Exploring the value of "humanised" mice

Looking to past failures - could we have predicted toxicity using modern in vivo tools?

Translation to human toxicity prediction

16:45

Evaluation of Microdosing Strategies Utilizing AMS and LC/MS-MS for ADME Studies in Drug Development
Punam Sandhu, Senior Investigator, Drug Metabolism & Pharmacokinetics, Merck

Linear kinetics of test compounds across microdose/sub-pharmacological and pharmacological dose ranges

Analytical tools to measure plasma concentrations over time to define kinetics at micro /sub pharmacological doses

Review of the available information on microdosing approaches and usefulness of such studies

17:20

Is There Too Much (Hot) Air in Genetic Toxicity Assessment?
Richard Walmsley, Professor of Genetics, The University Of Manchester

Does in vitro testing in atmospheric oxygen create misleading positive results?

ICH S2 (R1) test guidelines update: what is the appropriate top testing dose?

What is on the horizon for genotoxicity assessment? Maturing new technologies

17:55

Chairman’s Closing Remarks and Close of Day Two

Day one
Day two

ADMET

7 July - 8 July 2010 London, United Kingdom

Conference Overview

Conference agenda

8:30

Registration & Coffee

9:00

Chairman's Opening Remarks

9:05

ADME Optimisation in Early- and Late-Phase Drug Discovery

9:35

Targeting Drugs for the Brain

10:15

Morning Coffee

10:45

Probabilistic Model of Regioselectivity of Metabolism in Human Liver Microsomes

11:25

Vinblastine Treated CaCo-2 Culture as a Drug Penetration Model

11:55

Integrating Predictive ADMET into Hit to Lead and Optimisation

12:35

Networking Lunch

13:35

Structure-based ADMET Studies

14:05

RAPIDD plus

14:45

Building Hypotheses in Lead Selection and Optimisation

15:15

Afternoon Tea

15:45

Supersaturation Effects in Solubility-Enhancing Excipients and Biorelevant Media

16:20

Prediction of DDI's Arising from Cytochrome P450 Inhibition

16:50

Developing a Mechanism-based PK/PD Model

17:20

Drug Transporter Assays in Discovery

17:50

Chairman’s Closing Remarks and Close of Day One

8:30

Registration & Coffee

9:00

Chairman's Opening Remarks

9:10

The Utility and Application of TDI Screens in Early Discovery DMPK

9:45

System-dependent inhibition of cytochrome P450 (CYP) enzymes

10:25

Morning Coffee

10:55

Integrating Predictive Toxicology Model Development

11:40

Application of High Content Analysis for Predictive Cytotoxicity Testing & Preclinical Toxicity Biomarkers

12:15

Segregation of Genotoxic Compounds

12:50

Networking Lunch

13:50

In Vitro and In Vivo Approaches for Assessing the Potential for Drug Induced Liver Injury

14:25

Emerging In Vitro Toxicity Assays and the Role of Stem Cells in Assessing Human Toxicology

15:00

Mechanisms of Human (Hepato)Toxicity

15:40

Afternoon Tea

16:10

Metabolism-Based Drug Toxicity in Drug Development

16:45

Evaluation of Microdosing Strategies Utilizing AMS and LC/MS-MS for ADME Studies in Drug Development

17:20

Is There Too Much (Hot) Air in Genetic Toxicity Assessment?

17:55

Chairman’s Closing Remarks and Close of Day Two

Crowne Plaza Hotel - St James

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7 July - 8 July 2010
London, United Kingdom