2016 09-21 symposium opening the bbmri genomics infrastructure in the netherlands, amsterdam, alain...
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Biomarkers in Personalized Health(care): time for quality, not quantity
Prof Alain van Gool
BBMRI BIOS symposium Opening up the BBMRI genomics infrastructure in the Netherlands
21 September 2016, Amsterdam
A short story: Personalized medicine in melanoma
B-RAFV600E mutation Strong growth of cell Growth of tumor
• B-RAFV600E cells always grow and become cancer cells
• RAF inhibitors will block pathway, block cell growth and inhibit cancers that have a B-RAFV600E mutation
• 60% of melanoma patients have B-RAFV600E mutation
• Basis for a personalized medicine !
*
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Biomarkers to support clinical development
• Within Schering-Plough 4 Lead Optimisation programs in ERK pathway (2009)
• Need for blood-based biomarker that indicated downstream effects of drugs:
• Inhibition ERK pathway (pharmacodynamic)
• Tumor inhibition (efficacy)
• Extensive transcriptomics profiling: IL-8 as promising candidate biomarker
Data for RAFi #4
RAFi
MEKi
ERKi
RA
Fi #
1
RA
Fi #
2
RA
Fi #
3
RA
Fi #
4
MEK
i #1
MEK
i #2
ERK
i #1
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Validation study to confirm IL-8 in melanoma
Literature
{Yurkovetsky, et al. Clin Cancer Res, 2007}
Objectives: • Confirm elevated IL-8 in melanoma
• Develop IL-8 assays for clinical use
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Validation study to confirm IL-8 in melanoma
Stage 1 Stage 2 Stage 3 Stage 4
H&E staining; 20x
59 melanoma samples (tumor tissue (ffpe) + matching serum & plasma, stage I-IV, from two independent biobanks) + 40 healthy serum & plasma samples
1. Genetic analysis for BRAFV600E/D mutation in genomic DNA from tissue samples
2. IL-8 mRNA analysis in tissue samples by in situ hybridisation using bDNA probes (multiplexing with 12 ERK pathway response transcripts)
3. IL-8 protein analysis in tissue samples by immunohistochemistry (in parallel with 4 other ERK pathway response proteins, Ki67, Tunnel)
4. IL-8 protein analysis in matching plasma and serum by IL-8 immunoassay (3 formats: ELISA, Luminex, Mesoscale; singleplex and multiplex)
partial
OK
OK
?
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Validation study to confirm IL-8 in melanoma
Literature
{Yurkovetsky, et al. Clin Cancer Res, 2007}
Own data
{Unpublished, 2010}
Cause?
(6 months, 4 fte, USD 1.000.000)
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Lessons learned?
Source: Youtube - Burn after reading ending}
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Lessons learned?
Particularly for this case: 1. Know sample history
• IL-8 protein appeared sensitive to freeze-thawing
2. Know all relevant information from the source (patient) • Tumor load may be too low for our patients
3. Do these type of expensive validation studies together ! • For most pharma, biomarkers are precompetitive tools
We need a biomarker community that shares knowledge, ambitions, capabilities, successes, failures and best practice.
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Alain’s path 1989-now
• Molecular biology
• Mechanisms of disease
• Biomarkers
• Omics / technologies
• Translational medicine
• Personalized healthcare
Senior Scientist Integrator Biomarkers
Scientific lead DTL-Technologies
Head EATRIS Biomarker Platform
Professor of Personalized Healthcare Head Radboud Center for Proteomics, Glycomics & Metabolomics Coordinator Radboud Technology Centers
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Consider individual differences in life science research
10
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Source: Chakma, Journal of Young Investigators, 16, 2009
Principle of Personalized Medicine
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• The right drug for right patient at right dose at right time • Molecular biomarkers as key drivers of patient selection • = Precision medicine or Targeted medicine
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Personalized medicine in melanoma
Treat patients with
B-RAFV600E mutation Inhibit growth of cell
Patients live longer Tumors disappear Cells stop growing
B-RAF inhibitor
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Emerging Personalized / Precision / Targeted Medicine
2010:
5% of drugs in pipeline had companion diagnostic biomarker test
2015:
80%
50%
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Optimal Personalized / Precision / Targeted Medicine
Moving to personalized health(care)
{Source: Barabási 2007 NEJM 357; 4}
• People are more than linear pathways • Different systems and networks • Different risk factors • Different preferences
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Societal need in efficient personalized health(care)
{Source: prof Jan Kremer}
Towards cost effective care, less cure
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Highest need in efficient personalized health(care)
It’s personal !
‘I want to stay healthy.’ ‘If not, how do I get healthy?’
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Translating Personalized Health(care) in society
We need a personalized data-driven GPS for health
• Monitor (biomarkers) on background
• Alert when you are at risk
• Advice what to do
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3 key aspects of personalized health(care)
‘I want to stay healthy. If not, how do I get healthy?’
1. What to measure?
2. How much can it change?
3. What should be the follow-up for me?
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Exponential technological developments
• Next generation sequencing
• DNA, RNA • Risk analysis and therapy selection
• Mass spectrometry • Proteins, metabolites • Monitoring of disease and treatment effects
• Imaging
• Non invasive images, real time
• Spatial view of intact organs and organisms
500
1000
1500
2000
m/z
5 10 15 20 25 30 35 40 Time [min]
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Output from a proteomics biomarker lab • Mass spectrometry analysis of glycoproteins in human plasma • 0,05 microliter analysis: detection of 1.000.000 signals in one scan • ~40.000 peptides of which >80% contain sugar modification • Diagnose patients and identify new biomarkers
500
1000
1500
2000
m/z
5 10 15 20 25 30 35 40 Time [min]
Proof of principle study:
{Translational Metabolic Laboratory, Radboudumc, unpublished data}
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Challenge: translate laboratory to society
• Heart beat • Steps / movement • Glasses water/coffee • 1.000.000 molecules per analysis
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‘Self’ data (generated by patients, citizens)
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What does my DNA tell me?
23% chance blond hair 3.1% Neanderthaler DNA
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Genetic risk lung cancer → don’t smoke !
What does my DNA tell me?
No expected adverse reaction to Warfarin
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… but not all data is useful data !
Need for optimal quality in health biomarker analyses
Test, interpret, advice
“Post-traumatic Test Syndrome” ?
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3 key aspects of personalized health(care)
‘I want to stay healthy. If not, how do I get healthy?’
1. What to measure?
2. How much can it change?
3. What should be the follow-up for me?
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healthy disease disease + treatment
2. How much can it change?
Subgroups
100%
Individual
Population Past
Present
Future
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3 key aspects of personalized health(care)
‘I want to stay healthy. If not, how do I get healthy?’
1. What to measure?
2. How much can it change?
3. What should be the follow-up for me?
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3. What should be the follow-up for me?
Personal profile data
Knowledge
Understanding
(Shared) Decision
Action
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Biomarker innovation gaps !
Discovery Clinical
validation/confirmation
Diagnostic
test
Number of
biomarkers
Gap 1
Gap 2
Gap 3
• Too much biomarker discovery • Too little development to application
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Biomarker innovation gaps: some numbers
5 biomarkers/ working day
1 biomarker/ 1-3 years
1 biomarker/ 3-10 years
?
Eg Biomarkers in time: Prostate cancer May 2011: 2,231 biomarkers Nov 2012: 6,562 biomarkers Oct 2013: 8,358 biomarkers Nov 2014: 10,350 biomarkers Oct 2015: 11,856 biomarkers 12 Sept 2016: 13,888 biomarkers
Discovery Clinical
validation/confirmation
Diagnostic
test
Number of
biomarkers
Gap 1
Gap 2
Gap 3
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Reasons for biomarker innovation gap
• Not one integrated pipeline of biomarker R&D
• Publication pressure towards high impact papers
• Lack of interest and funding for confirmatory biomarker studies
• Hard to organize multi-lab studies
• Biology is complex on organism level
• Data cannot be reproduced
• Publishing bias towards extreme results
• Biomarker variability
• …
{Source: John Ioannidis, JAMA 2011}
{Source: Prinz, Schlange, Asadullah, Nat Rev Drug Disc 2011}
Slide from: Alain van Gool, Eur Commission advice, 11 Sept 2012
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Irreproducibility of data
{Freedman et al, PLOS Biology, 2015}
{2012} {2011} {2013} {2008} {2012}
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Categories of errors leading to irreproducibility
{Freedman et al, PLOS Biology, 2015}
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Add to this: bad Data Stewardship
{Wilkinson et al, Nature Scientific Data, 2016}
>80% of data is not FAIR:
Findable, Accessible, Interoperable, Reusable
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Way forward Quote Freedman paper:
{Freedman et al, PLOS Biology, 2015}
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Research Biomarkers Diagnostics
Department of Laboratory Medicine Integrated Translational Research and Diagnostic Laboratory, 250 fte, yearly budget ~ 28M euro. Close interaction with Dept of Genetics, Pathology, Pharmacy and Medical Microbiology
Specialities: • Proteomics, glycomics, metabolomics • Enzymatic assays • Neurochemistry • Cellulair immunotherapy • Immunomonitoring
Areas of disease: • Metabolic diseases • Mitochondrial diseases • Lysosomal /glycosylation disorders • Neuroscience • Nefrology • Iron metabolism • Pediatric oncology • Immunodeficiency • Transplantation
In development: • ~500 Biomarkers • Early and late stage • Analytical development • Clinical validation
Assay formats: • Immunoassay • Turbidicity assays • Flow cytometry • DNA sequencing • Mass spectrometry • Experimental human (-ized)
invitro and invivo models for inflammation and immunosuppression
Validated assays*: • ~ 1000 assays • 3.000.000 tests/year
Areas of application: • Personalized healthcare • Diagnosis • Prognosis • Mechanism of disease • Mechanism of drug action
Departmental community
*CCKL accreditation/RvA/EFI
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www.radboudumc.nl/research/technologycenters 43
Genomics
Bioinformatics
Animal studies
Stem cells
Translational neuroscience
Image-guided treatment
Imaging
Microscopy
Biobank
Health economics
Mass Spectrometry
Radboudumc Technology
Centers
Investigational products
Clinical studies
EHR data analysis
Statistics
Human performance
Data stewardship
Molecule
Flow cytometry
3D lab
Institutional community
National communities
(Centre for Translational Molecular Medicine) (Top Institute Pharma)
(BioMolecular Materials)
A rich history of public-private collaboration on diagnosis, drugs, devices (2006-2015)
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NL Biomarker validation pipelines
Standardisation, harmonisation, knowledge sharing in:
1. Assay development
2. Clinical validation
NL Roadmap Molecular Diagnostics (2012) NL Grant 4.3M Eur (2014)
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Ongoing independent biomarker activities
Europe
USA
{Asadullah et al, Nature Reviews Drug Discovery, Dec 2015}
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The Good Biomarker Practice initiative
Join forces among Europe’s major academic infrastructures + industry to:
1. Establish “Good Biomarker Practice” guidelines
- on translational research, biomarker technologies, biobanking, data stewardship.
2. Efficiently execute high quality biomarker projects
- work together in clinical validation and development of probable biomarkers.
47 Alain van Gool, Copenhagen Bioscience Lecture, 8 Sept 2016
National communities
Funding of Large scale Scientific Infrastructures (>10M euro)
Data4LifeSciences (organising biomedical data
in academic hospitals)
National Technology Infrastructure (from 40+ partners in DTL)
National Science Agenda (originated from citizens)
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www.onderzoeksfaciliteiten.nl
Nationale wetenschaps agenda
50
16
routes
51
Workshops March/April 2016 Output all routes presented as investment agenda to parliament 15 Sept 2016
Central thoughts Personalized Medicine route
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Emerging Health Research Infrastructure
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HealthRI: driving personalized medicine & health research in the Netherlands
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21-9-2016 55
Health-RI Congress
1 December 2016 De Flint in Amersfoort Aanmelden: www.nlhealthresearch.nl
Acknowledgements
Hans Wessels Jolein Gloerich
Roel Tans Esther Willems
Maurice van Dael Jenneke Keizer
Dirk Lefeber Monique van
Scherpenzeel
Leo Kluijtmans Ron Wevers
Marcel Verbeek Lucien Engelen
Jan Kremer Bas Bloem
Nathalie Bovy Paul Smits
the Radboudumc Technology Centers
and many others
www.radboudumc.nl/personalizedhealthcare
www.radboudumc.nl/research/technologycenters
www.radboudresearchfacilities.nl
www.linkedIn.com
www.slideshare.net/alainvangool
Many collaborators and funders
Jan van der Greef Ben van Ommen
Ivana Bobeldijk Hans Princen
Lars Verschuren Marjan van Erk
Suzan Wopereis Heleen Wortelboer
Wessel Kraaij Ronald Mooi
Peter van Dijken Cyrille Krul
and many others
CarTarDis
Ruben Kok Barend Mons
Jaap Heringa Merlijn van Rijswijk
and many others
Anton Ussi Florence Bietrix
Laura Bermejo Andreas Scherer
Sulev Koks Marian Hajduch
Giovanni Migliaccio
and many others
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