Download Molecular Diagnostics

Molecular Diagnostics:
Stanford University
y Medical
Center
February 10, 2009
1
Agenda
g
ƒ About XDx and Molecular
Diagnostics
ƒ R&D and
d P
Product
d t D
Development
l
t
ƒ AlloMap Molecular Expression
Testing
ƒ Challenges & Lessons Learned
2
2
About
Ab
XD and
XDx
d Molecular
M l
l
Diagnostics
Subtitle
3
XDx Mission
ƒ Mission
ƒ Improve patient care by developing
molecular diagnostics that translate an
individual’s immune status into clinically
actionable information
ƒ Goals
ƒ Understand the immune system on the
molecular level
ƒ Dynamically monitor the immune system
using genomics technologies and simple
blood test
ƒ Deliver clear and precise information to
clinicians making critical decisions where
no such information is currently available
4
Product Opportunities
ƒ Immune Mediated Inflammatory Diseases (IMID)
ƒ
Immune-system activation causes many inflammatory diseases:
Alloimmunity
y
400,000
Heart
Transplant
Lupus
Unpredictable course
Invasive biopsy
XDx
M ltiple
Multiple
Sclerosis
Autoimmunity
,
,
22,000,000
MRI imaging,
clinical
Lung
Transplant
Bronchial Lavage
Invasive biopsies
Renal
Transplant
Crohn’s
Disease
Colonoscopy, biopsy
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Blood tests followed by
biopsy
IMID Challenge
ƒ Delicate balance between
benefits
b
fit and
d side
id effects
ff t off
immunosuppressive therapy
ƒ Finding
Fi di the
th ““sweett spot”
t” h
has
been a challenge since the
advent of
i
immunosuppressive
i th
therapy
ƒ Lack of diagnostic innovation
6
Molecular Diagnostics
g
ƒ
Definition: the use of DNA, RNA, and proteins to
test for specific
p
states of health or disease
ƒ
Enabled by genomic technologies and information
ƒ Measurement technologies
ƒ DNA: PCR, hybridization
ƒ RNA: microarray, PCR
ƒ Protein:
antibodies, mass spec
ƒ Explosion of “analytes”—genes and gene products
ƒ
Allows detection of almost any biological state
7
7
The Business of Molecular
g
Diagnostics
ƒ
Diagnostics are valued based on how well the
information p
provided improves
p
clinical decisions
ƒ
Traditional diagnostics:
ƒ Known biology or associations of single
analytes (glucose, cholesterol, etc.)
ƒ Cheapest
p
and most efficient and convenient
technology wins…
ƒ
Molecular diagnostics:
ƒ Complicated biology of critical clinical
decisions can be addressed
ƒ Most innovative science and technical
implementation wins…
8
8
Examples of Successful Molecular
Diagnostics
g
ƒ
Myriad Genetics:
BRACAnalysis®
ƒ Assess inherited risk for breast cancer
ƒ Mutations in BRCA1 and BRCA2 by DNA sequencing
ƒ
Genomic Health:
Oncotype DX®
ƒ Predicts benefit of chemotherapy and risk of
recurrence in breast cancer patients
ƒ Gene expression levels of 21 genes from tumor
tissue
ƒ
Genentech: HER2/neu
ƒ Predicts response to Herceptin in breast cancer
patients
ƒ FISH (or IHC) detection of epidermal growth
factor 2 in tumors
Confidential, 3/6/2009
9
Opportunity to Change Medical Practice
ƒ Care focused on late-stage treatment: pathology, severe clinical
manifestations,, organ
g dysfunction
y
ƒ New diagnostic technologies: opportunity to reduce patient
morbidity and mortality, and health care costs by optimizing the
application of medical care
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R&D and Product
Development
Subtitle
Interdisciplinary
p
y Approach
pp
ƒ Developing molecular diagnostics requires
understanding
d t di th
the structure
t t
and
d properties
ti off
medical and biological information
1. Collecting and analyzing
genomic data
Clinical
2. Collecting and analyzing
clinical data
R&D
3. Correlating genomic
signatures with clinical
patterns
4 Distilling molecular
4.
signatures to provide
maximal clinical and
commercial value
12
Commercial
Information
Sciences
Corporate Technical
The Science: Gene Expression
g
Profiling
A. Trafficking of WBCs through tissues with acute rejection
B.
DNA - fixed genetic programming
RNA - dynamic gene expression
Protein - functional molecules
heart
activated
quiescent
Peripheral
p
blood
mononuclear cells
(PBMCs)
13
Wade N. RNA comes out of the shadow of its
famous cousin. Science Times. The
New York Times. June 21, 2005.
XDx Technologies
g
ƒ DNA Microarrays
ƒ Quantitative real-
time PCR
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XDx Technologies
g
ƒ DNA Microarrays
ƒ Quantitative real-
time PCR
ƒ Used for Discovery
(and confirmation of
biomarkers)
ƒ Used for Diagnostic
Test (Development
p
and
Validation)
ƒ Hybridization to
array of
oligonucleotides
sequences
ƒ Count PCR steps
i d t
to amply
l
required
from sample
ƒ Thousands of genes
ƒ Individually designed
(“whole genome”)
tested in single
experiment
specific and robust
assays
ƒ Increased sensitivity
ƒ Low sensitivity for
rare genes; low
specificity for
and reproducibility
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ƒ Accepted test
XDx Diagnostic Development
Process
I
Discovery
ƒ Product
P d t profile;
fil whole
h l genome analysis
l i and
d
literature; candidate gene selection and verification
II
Development
ƒ Classifier development; robustness and
performance; biomedical interpretation
III
Validation
ƒ Analytical and Clinical
Commercialization
IV
ƒ Establish clinical
utility & reimbursement
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AlloMap
All
M ® Molecular
M l
l
E
Expression
i
Testing
Subtitle
PATIENT
History & Physical
Exam
HEART
CELLULAR
Endomyocardial
Biopsy
Hemodynamics
18
Fluorescence (Molecu
ules)
Management of the Heart Transplant
Recipient
p
MOLECULAR
0
10
20
30
PCR Cycles
AlloMap Molecular
Expression Testing
40
Endomyocardial Biopsy
19
ISHLT Standardized Cardiac Biopsy Grading
Grade
2005
1990
0R
0
1R
3R
No rejection
1A
Focal perivascular and/or interstitial infiltrate without myocyte damage
1B
Diffuse infiltrate without necrosis
2
2R
Histopathological
p
g
Findings
g
One focus of infiltrate with associated myocyte damage
3A
Multifocal infiltrate with myocyte damage
3B
Diffuse infiltrate with myocyte damage
4
Diffuse, polymorphous infiltrate with extensive myocyte damage
Diffuse
± edema, ± hemorrhage, + vasculitis
Additional information (required when present): biopsy <4 pieces
pieces, humoral rejection,
rejection
“Quilty” effect, ischemia, infection present, lymphoproliferative disorder, other.
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Limitations of Endomyocardial Biopsy
ƒ Interpretive variability
Example of reader variability
ƒ IntraI t
and
d iinter-reader
t
d variability
i bilit
Agreement of Study Pathologists with Local
Pathologists (n=1,356)
ƒ Over calling of ≥3A
ƒ May miss focal areas of rejection
ƒ Repetitive biopsy leads to fibrosis
ƒ Invasive
ƒ Percutaneous catheterization
ƒ Risk (0.2-2.3%) includes:
ƒ Right ventricular perforation
ƒ Tricuspid valve damage
Average Study Patholo
ogist Agreemen
nt
ƒ Tissue sample
p inadequacy
q
y
100%
90%
80%
70%
60%
50%
40%
30%
20%
10%
0%
0
ƒ Arrhythmias
ƒ Bleeding
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1A, 1B
2
Local ISHLT Grade
3A, 3B
CARGO Study
y
ƒ
Hypothesis
ƒ Peripheral blood gene expression profiles can
differentiate between the absence and presence
of acute cellular rejection
ƒ
Study Overview
ƒ 9 center observational study
ƒ Columbia University (New York)
ƒ Cleveland
Cl
l d Cli
Clinic
i (Cl
(Cleveland)
l d)
ƒ Kaiser Permanente (San Jose)
ƒ Ochsner Clinic (New Orleans)
ƒ Stanford University (Palo Alto)
ƒ Temple University (Philadelphia)
ƒ UCLA (Los Angeles)
ƒ University of Florida (Gainesville)
ƒ University of Pittsburgh (Pittsburgh)
ƒ Conducted 2001-2005
ƒ 737 subjects
j
enrolled
ƒ 5,837 post transplant encounters
ƒ Centralized biopsy grading
ƒ 3 expert heart transplant pathologists read biopsies
ƒ Use of central reads to define Rejection/No rejection
(R/NR)
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AlloMap Discovery
ƒ
I
Definition of rejection
and non-rejection classes
ƒ Centralized pathology
data
ƒ
II
C ndid t Gene
Candidate
G n Selection
S l tion
ƒ Leukocyte microarray
analysis
ƒ 285 samples
III
ƒ 8,000 gene probes
ƒ Literature review,
database mining, expert
consultation
IV
ƒ
252 candidate
did t genes
selected
ƒ 23 68 biomarkers for
rejection verified by
Genes that Distinguish Rejection
ƒ
Quantitative real-time PCR for 252 candidate genes
ƒ
145 samples divided into ISHLT Grade 0 and ISHLT ≥3A by centralized pathologists
ƒ
68 genes correlated with rejection (p <0.01) or were more than 25% up- or down-regulated
Biopsy Grade 0
Biopsy Grade 3A
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AlloMap Development
Multi-gene classifier
development
ƒ
I
ƒ Statistically rigorous
ƒ Robust
II
ƒ Biologically plausible
20-gene linear classifier
derived by Linear
Discriminant Analysis
(LDA)
ƒ
III
ƒ 11 “informative” genes in
7 rejection pathways or
functional
i
groups
IV
ƒ 6 normalization genes
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Classifier Development
β0
+ β1 x Group1
Steroid Responsive
– β2 x Group 2
Platelet Activation
– β3 x Group3
Hematopoiesis
+ β4 x Gene 1
Morphology
+ β5 x Gene 2
T cell activation
+ β6 x Gene 3
T cell trafficking
g
+ β7 x Gene 4
B cell/T cell activation
26
AlloMap Validation
Clinical Verification
ƒ
I
ƒ
ƒ
II
ƒ
62 high-grade rejection
samples
86 mild rejection samples
122 no rejection samples
Analytical Validation
ƒ
III
ƒ
Reproducibility
ƒ
Confidence intervals
Over 800 additional samples in
order to characterize the
clinical performance
ƒ
IV
27
ƒ
NPV, PPV and score
distribution
ƒ
Longitudinal analysis
CARGO Clinical Validation Study
y Results
ƒ
AlloMap results significantly distinguish grade ≥3A
rejection from grade 0
(p <0.0001)
ƒ
Patients with low scores have very low risk of grade ≥3A
rejection on biopsy (e.g., beyond year 1, scores below 34
have an NPV of >99%)
ƒ
Patients with high scores have an increased but moderate
risk of current rejection (e.g. beyond year 1, scores above
h
have
a PPV of
f ~10%)
10%)
Confidential,
28
AlloMap Workflow
The sample needed for AlloMap testing can be obtained from a routine phlebotomy procedure. The prepared
sample is shipped, along with the completed test requisition form, to the XDx clinical laboratory for testing.
T t results
Test
lt are typically
t i ll reported
t d to
t the
th ordering
d i physician
h i i iin 1
1-2
2b
business
i
d
days.
29
AlloMap Value Proposition
ƒ AlloMap HTx addresses major clinical need in the long-
term management off heart transplant patients
ƒ Regular assessment of risk for acute cellular rejection used to
adjust management strategy (e
(e.g.
g immunosuppression)
ƒ Patients underwent frequent invasive endomyocardial biopsies as
only option pre-AlloMap
ƒ AlloMap HTx has substantial market potential (U.S. alone)
ƒ Over 15
15,000
000 commercial tests provided to date
ƒ Over 5,000 patients tested (~19,000 living recipients)
ƒ 75 transplant centers have ordered AlloMap (~150 in U.S.)
30
Challenges & Lessons
Subtitle
Confidential, 3/6/2009
31
“Crossing the Chasm”
ƒ Challenge: adoption of new technology is never simple
ƒ Even CARGO investigators didn’t immediately integrate AlloMap
ƒ Solutions & Lessons
ƒ Understand the perspectives (and psychology!) of all stake-holders
ƒ Patient,, Clinic,, Laboratory,
y, Reimbursement
ƒ Continue to show clinical value with strong science (IMAGE trial)
ƒ Education and training is the best marketing tool
ƒ Provide solutions or alternatives to your customer
32
Regulatory
ƒ Challenge: AlloMap was introduced as a Laboratory
Developed Test (LDT) under CLIA
CLIA, but the FDA now wants
to regulate as IVDMIA
ƒ Faced double regulatory burden starting in late 2006
ƒ Choice to engage or resist…
ƒ Solutions & Lessons
ƒ FDA clearance in August 2008
ƒ Reduce uncertainty through proactive engagement
ƒ You don’t need to be afraid if y
your science is strong
g
33
Reimbursement
ƒ Challenge: CMS changed a simple rule causing a
reimbursement upheaval
ƒ Date-of-service change meant hospitals had to bill Medicare for
tests on blood collected in the clinic
ƒ Financial risk shifted from XDx to hospital
ƒ Solutions
S l ti
&L
Lessons
ƒ Patient Service Centers (short term) and 3rd party solution
ƒ Stick to your core mission and business model
ƒ Consider all solutions
ƒ If you can’t change it, feature it!
34
Conclusions
ƒ A compelling mission and strong scientific culture serve as
the compass to navigate turbulent times
ƒ Invest your foundation and future in good times, and focus on what’s
important
p
for survival during
g bad times
ƒ Innovation = Invention + Implementation
ƒ Good science and clinical development are the foundation of any
biotechnology effort, but usually strategic and operational excellence
determines eventual success
ƒ An integrated, interdisciplinary approach is required at
multiple levels
35
Thank You!
Tod M. Klingler, Ph.D.
Vice President, Information Sciences
XDx
3260 Bayshore
y
Boulevard
Brisbane, CA 94005
tod@ xdx.com
415-287-2347
650-576-0577
Confidential, 3/6/2009
36