Table of Contents
1 Executive Summary: R&D Processes and Regulation for New Drugs, 2008-2020
- 1.1 Aim of this Report
- 1.2 Pharmaceutical Development and Regulation are Continually Evolving
- 1.3 An Overview of the Report
- 1.4 Economic Pressures and Regulatory Uncertainty
2 The Global Pharmaceutical Market Has Entered a Crucial Phase - Where Threats and Opportunities Meet
- 2.1 The Pharmaceutical Sector is a Leading Technological Industry:
However, It Faces Marked Economic Pressures
- 2.1.1 Number of Blockbusters Has Increased Along With Competition
- 2.1.2 Current Pressures on Industry - Blockbuster Business Model Under
the Spotlight
- 2.2 The World Pharmaceutical Market Continues to Grow, But Faces Mounting
Challenges
- 2.3 Pharmaceutical Development is a High Risk High Gain Business
- 2.3.1 R&D Strategy is Crucial to Success
- 2.4 The Continuing Success of the Pharmaceutical Industry is Dependent
upon Important Drivers and Restraints
- 2.5 Companies Are Gradually Changing Their Strategic Focus to Overcome
Challenges in the Worldwide Market
- 2.6 Unmet Needs and Specialist Uses Will Continue To Drive Innovation
- 2.7 Patent Protection Strategies Form a Cornerstone of Lifecycle Management
- 2.7.1 Falling Numbers of Drug Approvals are Accompanied by Fewer Patents
Submitted
- 2.7.2 Life Cycle Management Requires a Combination of Strategies
- 2.8 Drug Developers Face Increasingly Difficult Therapeutic Challenges
- 2.9 Increasing Developmental Times is a Serious Problem
- 2.10 Reducing Efficiencies in R&D Result in Concerns over Thinning
Pipelines
- 2.10.1 Is Innovation Declining in the Pharmaceutical Industry?
- 2.10.2 Follow-on Products are Very Appealing to Companies
- 2.10.3 Calls for a More-Collaborative Approach to Pharmaceutical
Regulation
- 2.10.4 Reform of Pharmaceutical Patenting Laws is Demanded
- 2.11 Healthcare Stakeholders Can Benefit from Radical Changes to
Regulatory Processes
- 2.12 Greater Regulatory Co-operation
- 2.13 Biomarkers and Theranostics
- 2.13.1 Pharmacogenomics is Increasingly Relevant to Pharmaceutical
Development
- 2.13.2 Proteomics Constitutes the "Next Step" After Genomics
- 2.13.3 Personalised Medicine Will Rely Heavily Upon Theranostics
- 2.13.4 The Completion of the Human Genome Project Has Been a Major
Driver of Molecular Diagnostics and Personalised Medicine
- 2.13.5 Personalised Medicine Supported by Theranostics Could Supersede
the Existing Blockbuster Model, With Sustainable Revenue Flows Continuing
- 2.14 Mandatory Price Reductions Continue to Beset the Pharmaceutical
Industry
- 2.14.1 There Are Strong Downward Pressures on Pricing Strategies
- 2.14.2 Pricing is a Key Issue - One that is Often Contentious
- 2.14.3 In Europe Governments are Exerting a Growing Influence on
Pharmaceutical Prices
- 2.14.4 It Is Possible That Mandatory Cost-Controls in Germany Will Serve
As a Precedent for Wider Governmental Controlling of Prices
- 2.14.5 Governmental Price Controls Are an Established Part of the
Japanese Pharmaceutical Market
- 2.15 Is the Blockbuster Business Model Sustainable?
3 Clinical Development and Approval of Pharmaceuticals in 2007
- 3.1 A Brief History of Clinical Trials
- 3.1.1 The Nuremberg Code and the Declaration of Helsinki
- 3.1.2 Establishing Standards for Good Clinical Practice and the
International Conference on Harmonisation (ICH)
- 3.2 Stages of Clinical Testing
- 3.2.1 Clinical Testing Follows a Rigorous Internationally-Recognised Code
- 3.2.2 Phase I Trials
- 3.2.3 Phase II Trials
- 3.2.4 Phase III Trials
- 3.2.5 Phase IV Trials (Post-Marketing Surveillance)
- 3.2.6 Further Division of Clinical Trials
- 3.3 Market Pressures are Driving the Need for Rationalisation of Clinical
Testing
- 3.4 The FDA - Gatekeepers to the Largest Pharmaceutical Market in the World
- 3.4.1 The FDA is the Most Important Pharmaceutical Regulatory Body in
the World
- 3.4.2 The CDER Oversees Drug Safety in the US
- 3.4.3 The FDA Is Under Pressure to Tighten-Up Drug Approval Procedures
- 3.4.4 Changes to Regulation of Off-Label Prescribing
- 3.5 The European Medicines Agency (EMEA) Controls a Diverse Range of
Countries
- 3.5.1 The EMEA Combines and Harnesses National Medical Expertise
- 3.5.2 The EMEA Makes the European Market More Accessible to Companies -
a Win-Win Situation
- 3.5.3 Structure of the EMEA
- 3.5.4 Approval Process of the EMEA and the EC
- 3.5.5 New Pharma Legislation in the EC
- 3.5.6 The EU Clinical Trials Directive
- 3.5.7 Provision for Joint Scientific Advice from the EMEA and FDA
- 3.5.8 Consultation Paper on Future of Healthcare in EU
- 3.6 Japan Has a High Level of Regulation
- 3.6.1 Approval of Foreign Pharmaceuticals in Japan was Traditionally a
Daunting Process
- 3.6.2 Japan has Rigorous Post-Marketing Drug Regulation
- 3.6.3 The Japanese System Accommodates Re-Evaluation of Drugs
- 3.7 Safety and Speed Are Now Pressing Issues for Regulatory Authorities
- 3.8 The Use of phase IV Clinical Trials Is Set to Increase Significantly
- 3.8.1 Post Marketing Surveillance is High on the Agenda Worldwide
- 3.8.2 Post Marketing Surveillance Can Benefit the Marketing of Products
- 3.8.3 Safety is Driving Phase IV Studies
- 3.8.4 Growth in Fast-Track Applications will also Stimulate Developments
in Post Marketing Studies
- 3.8.5 Self-Monitoring of Patients Will Become More Established
- 3.8.6 The UK Yellow Card System Is a Long-Established Example of
Post-Approval Monitoring
- 3.9 Stringent Assessment of Risk Will Require More Patients and Better
Indicators of Risk
- 3.10 Education Is a Key Issue
- 3.10.1 Public Mistrust of the Pharmaceutical Industry is a Serious
Problem
- 3.10.2 Problems with Vioxx and Other COX-2 Inhibitors Had a Major Impact
- 3.10.3 Open and Trustworthy Communication from both Companies and
Regulators is Vital
- 3.11 Changes in the Way Drugs Are Regulated Will Change the Nature of
Clinical Trials
- 3.12 Pharmacogenomics and Molecular Profiling Will Change Pharma
- 3.12.1 Pharmacogenomics Has the Potential to Revolutionise the
Pharmaceutical Industry
- 3.12.2 The Progress of Pharmacogenomics Has Been Slow
- 3.12.3 Identification of Expression Profiles in Pre-Clinical Models
- 3.12.4 A More Iterative Approach will Result in Greater Synergies in R&D
- 3.13 The Organisation of Clinical Testing is Changing
- 3.13.1 Phase I and II Clinical Trials Will Incorporate More Complex
Screening Techniques
- 3.13.2 Post-Regulatory Approval will Become More Prominent
- 3.14 Safety Concerns and Development Pressures Will Change the Structure
of Clinical Trials
4 How Pharmaceutical Development and Supporting Regulation Will Evolve from 2008 to 2020
- 4.1 Reducing Developmental Times and Late-Stage Failure are Crucial -
Developments in Testing and Regulation Will Aid the Process
- 4.1.1 Drugs Ineffectiveness in Sub-Populations is a Significant Obstacle
to Current Drug Development
- 4.1.2 There Are Steps that Can Reduce Developmental Times
- 4.1.3 R&D Will Change Due to New Developmental Models Supported by
Regulatory Reforms
- 4.1.4 Leading Industry Figures Call for More Flexible Approach to Drug
Approval
- 4.1.5 Regulators Acknowledge the Need for Stratification of Treatment
Populations
- 4.1.6 Visiongain Predicts Stratification of Patient Populations Leading
to Live-Licensing/In-Life Testing
- 4.1.7 There Will Be Greater Co-Operation between Regulators and
Pharmaceutical Developers from Now Onwards
- 4.1.8 Uncertainties over Political and Legislative Will to Achieve
Reform of Pharma Approval Processes
- 4.2 A SWOT Analysis for New Developments in the Pharmaceutical Market
Framework
- 4.2.1 SWOT Chart for Developmental and Regulatory Changes from 2008-2020
- 4.2.2 Efficient Use of Resources is Essential to R&D in the Years Ahead
- 4.2.3 Stratification of Patients is Key to More Personalised Medicine
Sought by Developers and Increasingly Required by Regulators
- 4.2.4 Traditional Clinical Development has a Significant Disadvantage -
Better-Targeted Studies will Take Precedence
- 4.2.5 Live Licensing/In-Life Testing is the Way Forward
- 4.2.6 Regulatory Systems are Already Becoming Closer Together - But
Global Convergence is Still Far from Certain
- 4.2.7 Electronic Patient Records Will Be an Important Facilitating Tool
of In-Life Testing
- 4.2.8 Evidence-Based Medicine will Become Increasingly Demanded by
Pharma Stakeholders
- 4.3 Adaptive Clinical Trial Design Will Facilitate Interaction with
Regulators and Provide Increased Rationalisation of Drug Development
- 4.3.1 Adaptive Clinical Trial Design Uses Accumulating Data
- 4.3.2 Regulators Should be Involved in the Process
- 4.3.3 Adaptive Trial Design will Gain Acceptance by Early Next Decade
- 4.4 Personalised Medicine Driven by Theranostics and Live
Licensing/In-Life Testing Will Become Established by 2020
- 4.4.1 Drivers for Better-Targeted Medicine
- 4.4.2 The Prospects for More-Personalised Medicine and Related
Diagnostics are Good
- 4.4.3 FDA Critical Path Initiative is a Progressive Move in the Right
Direction
- 4.5 Personalised Medicine Aided by Regulatory Reform will also Face
Significant Obstacles
- 4.5.1 The Complex, Disparate Pharma Industry Will Prove Difficult to
Reform, Especially in a Revolutionary Manner
- 4.5.2 It is Unclear How Extensively New Clinical Testing Models and
Supporting Regulation will be Applied
- 4.6 Calls for New Global Harmonization Effort from Influential Sources
- 4.6.1 Calls for Greater Regulatory Consensus
- 4.6.2 Agreements Between the FDA and EMEA are Already Taking Shape
Encouragingly
- 4.6.3 FDA-EC Co-Operation in Pharmacogenomics, Vaccines, Paediatric
Medicine, Oncology, Counterfeiting and Pharmacovigilance
- 4.6.4 Implementation Plan for Medicinal Products for Human Use and Other
Transatlantic Developments
- 4.6.5 Globalisation Facilitates Harmonisation of Pharmaceutical
Regulations
- 4.6.6 Design of a Supranational Regulatory Regime Should Protect
National Interests
- 4.6.7 Developing Nations Adopting ICH Guidelines
- 4.6.8 Increasing Willingness for Regulators to Collaborate on a Global
Scale - But No Sign of Global Regulatory Harmonisation
- 4.7 While Personalised Medicine and Better Targeted Clinical Trials are
Emerging, Such Developments are Welcomed by the FDA and EMEA
- 4.7.1 Emerging Developments are Welcomed by Pharma Stakeholders
- 4.7.2 Cancer Drug Development Leads the Way in its Merging of Drug
Development and Treatment of the Disease
- 4.7.3 FDA' s Critical Path Initiative and Personalised Medicine
- 4.7.4 Theranostic Solutions Will Aid the Development of Personalised
Medicine and Improve Support from Regulators through Evidence-Based Medicine
- 4.8 Pricing of Personalised Medicine
- 4.8.1 Personalised Medicine will Lead to Changes in Pricing and
Reimbursement
- 4.8.2 Onus is on Companies to Prove Benefits of their Drugs Including
Comparative Cost-Benefits
- 4.8.3 Biomarkers Can Create Value
- 4.8.4 Non-Compliance is a Major Problem that Can be Ameliorated via
More-Personalised Medicine
- 4.8.5 The Developments are Complex and Systemic, Posing both
Opportunities and Challenges for Healthcare Stakeholders
- 4.9 Evidence-Based Medicine and Pharmacoeconomic Analyses
- 4.9.1 Comparative Testing is Prevalent
- 4.9.2 Electronic Medical Records are a Major Priority for Leading Nations
- 4.9.3 GSK Leads Way in Evidence-Based Medicine
- 4.9.4 Personalised and Evidence-Based Medicine Will Require Time for
Acceptance
- 4.10 Changes to Regulation Governing Paediatric Medicine
- 4.11 Visiongain Believes that the New Developments Will Cut Developmental
Time and Provide Better Healthcare
- 4.11.1 Shift from General to Personalised Healthcare is an Inevitable
Trend with Significant Potential Gains for Industry and Society
- 4.11.2 Increased Use of Conditional Acceptance Based upon Live Licensing
and In-Life Testing Constitute a Logical Progression
- 4.11.3 Pharmaceutical Developers Must Understand the Needs and
Preferences of Other Healthcare Stakeholders
5 Emerging Technology Will Underpin Changes to Developmental Processes and Regulatory Policy
- 5.1 Personalised Medicine is a Prime Aim for Healthcare
- 5.1.1 An Introduction to Pharmacogenomics
- 5.1.2 The Aim of Pharmacogenomics
- 5.1.3 Pharmacogenomic Drugs as Personalised Medicines
- 5.1.4 The Economic Potential of Pharmacogenomics
- 5.2 The Advantages of Pharmacogenomics Drugs and Benefits to the
Pharmaceutical Industry
- 5.2.1 Pharmacogenomics is Attracting a Great Deal of Interest from
Pharma Stakeholders
- 5.2.2 Improved Drugs Through Better Targeting
- 5.2.3 Reduced Deaths from Adverse Drug Reactions
- 5.2.4 Personalised Drugs are More Likely to Work Safely and Efficaciously
- 5.2.5 Advanced Screening for Disease Leading to Quicker Diagnoses
- 5.2.6 Improved Vaccines
- 5.2.7 Improvements in Drug Discovery and Reduced Cost of Clinical Trials
- 5.3 Adverse Drug Reactions are a Serious Problem
- 5.3.1 Economic and Other Consequences of ADRs
- 5.3.2 ADR and Genotype: Tacrine, a Case Study
- 5.4 The Human Genome Project (HGP) and its Influence on Pharmacogenomics
- 5.5 Barriers to the Growth of Pharmacogenomics
- 5.5.1 The Complexity of Finding SNP Gene Variations that Affect Drug
Responses
- 5.5.2 Limited Therapeutic Alternatives
- 5.5.3 Disincentives for Drug Companies to Develop and Produce Multiple
Treatments for a Disease
- 5.5.4 Educating Healthcare Providers
- 5.6 Advances in Computing and Electronic Communications Will Benefit
Pharmaceutical R&D
- 5.6.1 There are Prominent Examples of Electronic Solutions Benefiting
Pharmaceutical Development
- 5.6.2 Electronic Data Capture (EDC) Promises to Streamline Clinical
Trials
- 5.6.3 Training and Security are Barriers to EDC Conversion
- 5.6.4 The Clinical Trials Industry Must Take the Initiative on EDC
Standards
- 5.6.5 Governments Working Hard to Establish e-Health Records
- 5.7 Electronic Submission of Post-Marketing Safety Data is Another
Important Development
- 5.8 Proteomics Constitutes the "Next Step" After Genomics
- 5.9 Advanced Diagnostics Will Aid Personalised Medicine and In-Life Testing
- 5.9.1 Theranostics - The Combination of Therapy and Diagnostics
- 5.9.2 Exciting Developments in Molecular Biology Can Bring Two
Healthcare Industries Closer Together
- 5.9.3 Personalised Medicine Will Rely Heavily Upon Theranostics
- 5.9.4 Theranostic Applications Will Exhibit Rapid Market Growth from
2007-2012
- 5.9.5 Personalised Medicine Will Become More Prominent in Healthcare
with Theranostics Benefiting as a Result
- 5.9.6 The Completion of the Human Genome Project Has Been a Major Driver
of Molecular Diagnostics
- 5.9.7 Personalised Medicine Supported By Theranostics Could Supersede
the Existing Blockbuster Model, With Sustainable Revenue Flows Continuing
- 5.9.8 Theranostics will Benefit from FDA' s Guidance on Pharmacogenomic
Data Submission
- 5.9.9 Distinguishing Patients at a Greater Risk is Vital
- 5.9.10 In Future Parallel Use of Markers and Drugs Will Become Prevalent
- 5.9.11 The EDMA Cites Theranostics as a Medium-to-Long-Term Driver for
Healthcare
- 5.9.12 Personalised Medicine is a Strong Driver of the Theranostics
Sector
- 5.9.13 While Personalised Medicine Is Still a Goal for the Future, the
Technology Is Already Emergent
- 5.9.14 Identifying Suitable Biomarkers Remains a Significant Challenge
- 5.9.15 Theranostics Bill Introduced in the US Senate During 2006
- 5.9.16 Funding for Theranostics R&D Efforts May Be Limited by Low
Reimbursement Rates
- 5.9.17 Cancer Diagnostics is an Important Growth Area with Relevance to
Theranostics
- 5.9.18 Collaboration among Stakeholders is Essential
- 5.9.19 Intra-Industry Collaboration is Important to Achievement of
Innovation in the Years Ahead
- 5.9.20 Nucleic Acid Testing Will Be Decisive in the Development of the
Theranostics Market
- 5.9.21 The Outlook for Theranostics
6 Interviews with Experts in Pharmaceutical Regulatory Affairs: Drug Development - Present and Future Trends
- 6.1 Respondent 1: US-Based Academic Specialising in US Pharmaceutical
Regulation
- 6.1.1 The Most Important Unmet Regulatory Needs
- 6.1.2 What Changes are Going to Occur?
- 6.1.3 Will the Changes Become Widespread, Geographically and in Disease
Area?
- 6.1.4 Potential Resistance from Payers
- 6.1.5 How Will Pharma R&D Benefit?
- 6.1.6 The Obstacles to Regulatory Reform
- 6.2 Respondent 2: US-Based Academic Specialising in International
Pharmaceutical Regulation
- 6.2.1 The Most Important Unmet Regulatory Needs
- 6.2.2 What Changes are Going to Occur?
- 6.2.3 Will the Changes Become Widespread, Geographically and in Disease
Area?
- 6.2.4 Potential Resistance from Payers
- 6.2.5 How Will Pharma R&D Benefit?
- 6.2.6 The Obstacles to Regulatory Reform
- 6.3 Respondent 3: Analyst from a European Pharmaceutical Industry
Representative Group
- 6.3.1 The Most Important Unmet Regulatory Needs
- 6.3.2 What Changes are Going to Occur?
- 6.3.3 Will the Changes Become Widespread, Geographically and in Disease
Area?
- 6.3.4 Potential Resistance from Payers
- 6.3.5 How Will Pharma R&D Benefit?
- 6.3.6 The Obstacles to Regulatory Reform
- 6.4 Respondent 4: US-Based Academic Specialising in US and European
Pharmaceutical Regulation
- 6.4.1 The Most Important Unmet Regulatory Needs
- 6.4.2 What Changes are Going to Occur?
- 6.4.3 Will the Changes Become Widespread, Geographically and in Disease
Area?
- 6.4.4 Potential Resistance from Payers
- 6.4.5 How Will Pharma R&D Benefit?
- 6.4.6 The Obstacles to Regulatory Reform
- 6.5 Respondent 5: Regulatory Affairs Analyst from an International
Business Consultancy Specialising in the Pharmaceutical Industry
- 6.5.1 The Most Important Unmet Regulatory Needs
- 6.5.2 What Changes are Going to Occur?
- 6.5.3 Will the Changes Become Widespread, Geographically and in Disease
Area?
- 6.5.4 Potential Resistance from Payers
- 6.5.5 How Will Pharma R&D Benefit?
- 6.5.6 The Obstacles to Regulatory Reform
- 6.6 Respondent 6: Representative from Regulatory Affairs in an
International Pharmaceutical Company
- 6.6.1 The Most Important Unmet Regulatory Needs
- 6.6.2 What Changes are Going to Occur?
- 6.6.3 Will the Changes Become Widespread, Geographically and in Disease
Area?
- 6.6.4 Potential Resistance from Payers
- 6.6.5 How Will Pharma R&D Benefit?
- 6.6.6 The Obstacles to Regulatory Reform
- 6.7 Respondent 7: Head of Regulatory Affairs in a Top-10 Pharmaceutical
Company
- 6.7.1 The Most Important Unmet Regulatory Needs
- 6.7.2 What Changes are Going to Occur?
- 6.7.3 Will the Changes Become Widespread, Geographically and in Disease
Area?
- 6.7.4 Potential Resistance from Payers
- 6.7.5 How Will Pharma R&D Benefit?
- 6.7.6 The Obstacles to Regulatory Reform
7 Conclusions of this Study
- 7.1 The Prevailing Development of Pharmaceuticals is Under Increasing
Commercial and Regulatory Pressure
- 7.2 Pharmaceutical Regulatory Authorities Play a Vital Role in Healthcare
- 7.3 Personalised Medicine and Rationalisation of the Developmental Process
- 7.4 Developmental Processes and Regulatory Policy Need to Accommodate
Stratified Patient Populations
- 7.5 Visiongain Predicts Stratification of Patient Populations Leading to
Live-Licensing/In-Life Testing
- 7.6 There Will Be Greater Co-Operation between Regulators and
Pharmaceutical Developers
- 7.7 Uncertainties over Political and Legislative Will to Achieve Reform of
Pharma Approval Processes
- 7.8 Greater Regulatory Co-Operation - However, No Sign of Global
Harmonisation in Pharma in Sight
- 7.9 Theranostic Solutions Will Aid the Development of Personalised
Medicine and Improve Support from Regulators through Evidence-Based Medicine
- 7.10 Increased Use of Conditional Acceptance Based upon Live Licensing and
In-Life Testing Constitute a Logical Progression from 2008-2020
Appendix A: Glossary
Appendix B: About visiongain
Appendix C: visiongain report evaluation form
List of Tables
- Table 2.1 Major Drugs Losing Patent Expiry in Near Future
- Table 2.2 Revenue Generation ($bn) by the World Pharmaceutical Industry,
2000-2006
- Table 2.3 Forecast Revenue Generation ($bn) by the World Pharmaceutical
Market, 2006-2012
- Table 3.1 Key Stages in the History of Clinical Trials
- Table 3.2 Drug Approvals Agencies within the EU
- Table 4.1 Greater Use of Disease Knowledge and Biomarkers Will Benefit
Pharmaceutical Development
- Table 4.2 SWOT Chart for Developmental and Regulatory Changes, 2008-2020
- Table 4.3 Visiongain' s Predictions of How Changes to Pharma Development
Will Benefit the Industry and Other Stakeholders, 2007-2020
- Table 5.1 Assessment of EDC Solutions
- Table 5.2 Share (%) of the World Molecular Diagnostics Market Held by
Theranostics, 2006 & 2012
List of Figures
- Figure 2.1 Revenue Generation ($bn) by the World Pharmaceutical Industry,
2000-2006
- Figure 2.2 Forecast Revenue Generation ($bn) by the World Pharmaceutical
Market, 2006-2012
- Figure 2.3 The Drug Development Process is Long, Complex and Costly
- Figure 2.4 Increasing Average Cost ($m) of NCE Development, 1976-2005
- Figure 4.1 The Current Framework for Drug Development
- Figure 4.2 How Pharmaceutical Development Will Evolve into a More
Progressive System
- Figure 4.3 The Dynamic Integrated Regulatory System of the Future
- Figure 4.4 Systemic Changes to Pharmaceutical Regulation Involve all
Healthcare Stakeholders
- Figure 5.1 Progressive Technological Developments in Medicine
- Figure 5.2 World Revenues ($m) for Theranostic Applications, 2006-2012
Companies Mentioned in this Report
- Abbott Laboratories
- Affymetrix
- Amgen
- AstraZeneca
- Bayer HealthCare
- Cambridge Antibody Technologies
- Chiron
- CyGene
- Dako
- Digene
- Eli Lilly
- EXACT Sciences
- First Horizon
- Genaissance Pharmaceuticals
- Genentech
- Genetic Vectors
- Gen-Probe
- Glaxo Wellcome
- GlaxoSmithKline
- Hoechst Marion Roussel
- Human Genome Sciences
- IGEN International
- Innogenetics
- Millennium Pharmaceuticals
- Myriad Genetics
- Organon
- Pfizer
- Roche
- Sanofi-Aventis
- Schering Plough
- Sequenom
- Teknika
- Tibotec-Virco
- Visible Genetics
- Vysis
- Warner Lambert
- Wyeth
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