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Quantitative Assessment of Tissue-based IHC Biomarkers
25 March 2017 Quantitative Assessment of Tissue-based IHC Biomarkers Next Generation Pharmaceutical Summit David Young Apr 09 New Targets Committee
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Digital Pathology 25 March 2017 Digital Pathology – Research and Clinical Possibilities Quantitative Digital pathology IHC – Traditional evaluation vs Image analysis Tools not limited to pathologists New Targets Committee
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Digital Pathology – Where Are We Headed?
25 March 2017 Digital Pathology – Where Are We Headed? New Targets Committee
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Digital Pathology 25 March 2017 Digital Pathology – Research and Clinical Possibilities Archival of pathology specimens Diagnosis Digital slide conferencing Consultation Help from Development Teams putting the power in the hands of the people who know it best New Targets Committee
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Quantitative Digital Pathology - The Next Step
25 March 2017 Quantitative Digital Pathology - The Next Step New Targets Committee
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Quantitative Digital Pathology
25 March 2017 Pathologist opinions Good enough for government work, or Close, but no cigar X number of pathologists = Y number of results Diagnoses IHC analysis subjective; based on familiarity of tissue and experience New Targets Committee
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IHC Assessment of Tissue-based Biomarkers
25 March 2017 IHC Assessment of Tissue-based Biomarkers New Targets Committee
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Immunohistochemistry Analyses and Quantitative Digital Pathology
25 March 2017 Not an exact science Basis of many aspects of drug development and drug selection New Targets Committee
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Biomarker Scoring Consensus
25 March 2017 Biomarker Scoring Consensus Clark (2006) – ‘there is no consensus in the literature about how to summarize these scoring assessments into a single determination of EGFR protein expression status as EGFR positive or EGFR negative.’ ‘Evaluation of the clinical significance of EGFR expression by IHC has been complicated by the use of different antibodies, different scoring systems, and different clinical endpoints.’ Clark, et al: J Thorac Oncol 2006 New Targets Committee
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Importance of Standardized Scoring
25 March 2017 Prevalence and tumor surveillance Prognostic factors Predictive factors Comparing study results from a recognized baseline of analysis New Targets Committee
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IHC Scoring Concordance – Pathologists Variability
25 March 2017 Concordance Total scoring = 78% Cut point <100 = 92% Concordance Total scoring = 75% Cut point <100 = 100% New Targets Committee
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Pathologist Variation
25 March 2017 Legend: Red – Pathologist 1 Blue – Pathologist 2 Pathologist 1 Scores: Y = 0.96X R = 0.987 Pathologist 2 Scores: Y = 0.97X -2.72 R = 0.974 New Targets Committee
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Image Analysis – Lessens Subjectivity of Scoring
25 March 2017 Quantify: Size (area) Positive cells Negative cells Intensity levels New Targets Committee
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Tissue-based Biomarkers – Case Study
25 March 2017 E-Cadherin Marker of epithelial phenotype Associated with cell-to-cell adhesion Membrane protein Vimentin Marker of mesenchymal phenotype Associated with cellular skeleton Cytoplasmic protein New Targets Committee
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Experimental Xenograft model
25 March 2017 H&E E-cad Vim New Targets Committee
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Heterogeneity in Tumor Tissue – E-cad
25 March 2017 New Targets Committee
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Heterogeneity in Tumor Tissue – Vim
25 March 2017 New Targets Committee
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Traditional IHC Score (H-Score)
25 March 2017 Traditional IHC Score (H-Score) 1% 10% 30% 75% 100% Proportion Score (PS) 0 – 100% Immunostaining was scored using a previously established scoring system developed by Dr. Craig Allred in our group. The proportion of stained tumor cells was estimated on a scale of 0 to 5: 0 represents no staining; 1 is less than 1/100 cells; 2 is 1/100 to 1/10 cells; 3 is 1/10 to 1/3; 4 is 1/3 to 2/3; and 5 indicates staining in more than 2/3 of the tumor cells. Staining intensity was rated as negative, weak, intermediate, or strong. A total IHC score was calculated by adding the proportion score and the intensity score. The range of values is 0, and 2 to 8. Intensity Score (IS) 0 = negative 1 = weak 2 = intermed 3 = strong Score range: 0-300 New Targets Committee
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Factors Affecting IHC Analysis – Not Just the Pathologist
25 March 2017 Tumor acquisition (pre-analytical factors) Tumor size Tumor type (Tumor tissue and host response) Antibodies Processing factors Individual variation in evaluation New Targets Committee
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Cell Culture - E-cadherin
25 March 2017 Algorithm - Membrane v9 Default Min Nuclear Size (um^2) 10 85 Background Intensity Threshold 240 Weak (1+) Intensity Threshold 200 Moderate (2+) Intensity Threshold 170 Strong (3+) Intensity Threshold 105 New Targets Committee
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NSCLC Criteria setup 25 March 2017 New Targets Committee
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Cell Culture - Vimentin
25 March 2017 Algorithm - Color Deconvolution v9 Default Weak Postive Threshold 220 180 Medium Postive Threshold 175 120 Strong Positive Threshold 100 60 New Targets Committee
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Xenograft model - E-cadherin
25 March 2017 Entire Specimen IHC Test box (3+) Percent Cells 71.83 50 65.67 (2+) Percent Cells 9.61 40 8.17 (1+) Percent Cells 18.53 10 26.16 (0+) Percent Cells 0.03 0.00 SCORE 253.24 240 239.51 New Targets Committee
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Xenograft model - Vimentin
25 March 2017 Entire Specimen IHC Test box (3+) Percent 41.28 25 24.70 (2+) Percent 46.02 50 56.80 (1+) Percent 20 17.51 (0+) Percent 0.26 5 1.00 SCORE 228.32 195 205.21 New Targets Committee
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NSCLC – example 1 25 March 2017 New Targets Committee
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NSCLC – example 1 (higher mag)
25 March 2017 E-Cad Vim Aperio IHC (3+) Percent Cells 41.28 25 (3+) Percent 1.10 1 (2+) Percent Cells 46.02 50 (2+) Percent 0.96 (1+) Percent Cells 20 (1+) Percent 3.03 3 (0+) Percent Cells 0.26 5 (0+) Percent 94.90 95 SCORE 228.32 195 8.25 8 New Targets Committee
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NSCLC – example 2 25 March 2017 New Targets Committee E-Cad Vim Aperio
IHC (3+) Percent cells 61.77 35 (3+) Percent 6.93 (2+) Percent cells 17.73 60 (2+) Percent 30.51 10 (1+) Percent cells 20.00 5 (1+) Percent 43.15 30 (0+) Percent cells 0.50 (0+) Percent 19.41 SCORE 240.77 230 124.96 50 New Targets Committee
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NSCLC – example 3 25 March 2017 New Targets Committee E-Cad Vim Aperio
IHC (3+) Percent Cells 65.28 15 (3+) Percent 3.80 (2+) Percent Cells 9.88 (2+) Percent 2.21 10 (1+) Percent Cells 24.80 50 (1+) Percent 6.05 (0+) Percent Cells 0.04 20 (0+) Percent 87.94 75 SCORE 240.40 125 21.87 35 New Targets Committee
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NSCLC – example 4 (Whole tumor; E-Cadherin)
25 March 2017 E-Cad Aperio IHC (3+) Percent Cells 68.60 50 (2+) Percent Cells 6.25 25 (1+) Percent Cells 24.54 20 (0+) Percent Cells 0.60 5 SCORE 242.84 220 New Targets Committee
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NSCLC – example 4 (Vimentin)
25 March 2017 Vim Aperio IHC (3+) Percent 0.44 (2+) Percent 0.96 (1+) Percent 2.50 (0+) Percent 96.11 100 SCORE 5.74 New Targets Committee
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Pancreas – Xenograft 1 H&E E-cad Vim 25 March 2017
New Targets Committee
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Pancreas – Xenograft 1 25 March 2017 New Targets Committee E-Cad Vim
Aperio IHC (3+) Percent Cells 71.59 50 (3+) Percent 0.40 (2+) Percent Cells 7.48 40 (2+) Percent 1.26 (1+) Percent Cells 20.93 10 (1+) Percent 24.36 (0+) Percent Cells (0+) Percent 73.98 100 SCORE 250.66 240 28.08 New Targets Committee
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Pancreas – Xenograft 2 25 March 2017 New Targets Committee E-Cad Vim
Aperio box Aperio whole IHC (3+) Percent Cells 0.76 (3+) Percent 50.82 51.80 70 (2+) Percent Cells 10.65 (2+) Percent 34.35 34.72 30 (1+) Percent Cells 22.22 49.27 (1+) Percent 13.26 12.42 (0+) Percent Cells 77.78 39.32 100 (0+) Percent 1.58 1.06 SCORE 72.85 234.42 237.26 270 New Targets Committee
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Summary – What have we learned so far?
25 March 2017 Selection of site for IHC evaluation is important; may or may not be reflective of whole tumor Tumor heterogeneity affects tissue-based biomarker assessment and analysis IA correlates well with traditional IHC scoring methods. Validation removes pathologists scoring variability ‘Tweaking’ of algorithms required prior to universal deployment New Targets Committee
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Putting the Power in the Hands of the People
25 March 2017 Putting the Power in the Hands of the People New Targets Committee
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Investigator Asks the Questions
25 March 2017 New Targets Committee
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25 March 2017 Thank you! New Targets Committee
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