Download PPT - National Coalition for Cancer Research

Survey
yes no Was this document useful for you?
   Thank you for your participation!

* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project

Document related concepts
no text concepts found
Transcript
Cancer Treatment from the DNA
Perspective
Peter J. O’Dwyer, MD
University of Pennsylvania
ECOG-ACRIN
Cancer Research Group
DNA Mutation
DNA
CA AG C T A A C T
Normal gene
CA AG C G A A C T
Single base change
CA A G G CG C T A A C T
Additions
C
T
CA A G A A C T
Deletions
Oncogenes
Normal cell
Cancer cell
Mutated/damaged oncogene
Normal
genes
regulate
cell growth
Oncogenes
accelerate
cell growth
and division
Tumor Suppressor Genes
Act Like a Brake Pedal
Tumor Suppressor
Gene Proteins
Growth factor
Receptor
Signaling
enzymes
Cell nucleus
Transcription
factors
DNA
Cell proliferation
Genomics-Driven Trials
• Assumption: Given a specific mutation, a particular
growth or survival pathway will be activated, so
therapy can be directed specifically to it
• Disease-Specific
– Breast Cancer – I-SPY
– Lung Cancer – LUNG-MAP, ALCHEMIST
– Colorectal Cancer – ASSIGN (in development)
• “Disease-Agnostic”
– MATCH
MATCH – Preliminary Hypothesis
Primary:
That tumors that share common somatic genetic
alterations in oncogenes will be variably responsive to
therapies targeting the oncogenic pathway based on
lineage specific factors.
Secondary:
That concomitant somatic genetic alterations will predict
responsiveness or resistance.
6
MATCH TRIAL OVERVIEW
•
•
•
•
Identify mutations/amplifications/translocations in patient
tumor sample - eligibility determination
Assign patient to relevant agent/regimen – single-arm
Phase II design
Need to sequence large numbers of tumors (3000pts) and
need to have large numbers of targeted treatments
Tumor biopsies & sequencing at progression to
investigate resistance mechanisms
– De-identified samples submitted to central labs
– Whole-exome sequencing (research purposes) to detect
non-ambiguous germline variants
Alliance Spring Group Meeting / May 9, 2014
7
MATCH: SCHEMA
Tumor Biopsy
Statistical Considerations
Within each drug-by-mutation category:

Dual Primary Endpoints:

Overall Response Rate 5% vs. 25% or

Progression Free Survival 6 months 15%
(median PFS 2.2 m) vs 35% (median PFS 4 m)

One stage design 31 evaluable patients per arm
ORR = proportion of patients with objective response (PR+CR) on initial
course of study agent
PFS6 = proportion of patients alive and progression free at 6 months
from initiation of study agent
9
CLIA LAB NETWORK
• Genetic platform: Ion Torrent PGM AmpliSeq custom
panel; Oncomine under evaluation
– About 200 genes
– SNV, indel, CNV, targeted translocations
• Immunohistochemical expression of PTEN
• Validation within and across sites: same SOP
• Possibly additional IHC and FISH, if needed
• Lead laboratory: Frederick National Laboratory for
Cancer Research (Williams)
– Competitively chosen lab sites:
• MD Anderson (Hamilton)
• MGH (Iafrate)
• Yale (Sklar)
SUMMARY
• In planning for a year, MATCH slated to open by
end 2014.
• Robust state-of-the-art platform finalized
September 2014
• Agreements close to final with four companies for
genotype-specific drugs
• Strong CTEP-Intergroup collaboration in
developing the trial
• Broad community oncologist and advocate input
refined design
11
NCI MATCH
PARTICIPATION