@synsci/cli-darwin-x64 1.1.97 → 1.1.99

This diff represents the content of publicly available package versions that have been released to one of the supported registries. The information contained in this diff is provided for informational purposes only and reflects changes between package versions as they appear in their respective public registries.
Files changed (1549) hide show
  1. package/bin/synsc +0 -0
  2. package/package.json +1 -1
  3. package/bin/skills/accelerate/SKILL.md +0 -332
  4. package/bin/skills/accelerate/references/custom-plugins.md +0 -453
  5. package/bin/skills/accelerate/references/megatron-integration.md +0 -489
  6. package/bin/skills/accelerate/references/performance.md +0 -525
  7. package/bin/skills/adaptyv/SKILL.md +0 -114
  8. package/bin/skills/adaptyv/reference/api_reference.md +0 -308
  9. package/bin/skills/adaptyv/reference/examples.md +0 -913
  10. package/bin/skills/adaptyv/reference/experiments.md +0 -360
  11. package/bin/skills/adaptyv/reference/protein_optimization.md +0 -637
  12. package/bin/skills/aeon/SKILL.md +0 -374
  13. package/bin/skills/aeon/references/anomaly_detection.md +0 -154
  14. package/bin/skills/aeon/references/classification.md +0 -144
  15. package/bin/skills/aeon/references/clustering.md +0 -123
  16. package/bin/skills/aeon/references/datasets_benchmarking.md +0 -387
  17. package/bin/skills/aeon/references/distances.md +0 -256
  18. package/bin/skills/aeon/references/forecasting.md +0 -140
  19. package/bin/skills/aeon/references/networks.md +0 -289
  20. package/bin/skills/aeon/references/regression.md +0 -118
  21. package/bin/skills/aeon/references/segmentation.md +0 -163
  22. package/bin/skills/aeon/references/similarity_search.md +0 -187
  23. package/bin/skills/aeon/references/transformations.md +0 -246
  24. package/bin/skills/alphafold-database/SKILL.md +0 -513
  25. package/bin/skills/alphafold-database/references/api_reference.md +0 -423
  26. package/bin/skills/anndata/SKILL.md +0 -400
  27. package/bin/skills/anndata/references/best_practices.md +0 -525
  28. package/bin/skills/anndata/references/concatenation.md +0 -396
  29. package/bin/skills/anndata/references/data_structure.md +0 -314
  30. package/bin/skills/anndata/references/io_operations.md +0 -404
  31. package/bin/skills/anndata/references/manipulation.md +0 -516
  32. package/bin/skills/arboreto/SKILL.md +0 -243
  33. package/bin/skills/arboreto/references/algorithms.md +0 -138
  34. package/bin/skills/arboreto/references/basic_inference.md +0 -151
  35. package/bin/skills/arboreto/references/distributed_computing.md +0 -242
  36. package/bin/skills/arboreto/scripts/basic_grn_inference.py +0 -97
  37. package/bin/skills/astropy/SKILL.md +0 -331
  38. package/bin/skills/astropy/references/coordinates.md +0 -273
  39. package/bin/skills/astropy/references/cosmology.md +0 -307
  40. package/bin/skills/astropy/references/fits.md +0 -396
  41. package/bin/skills/astropy/references/tables.md +0 -489
  42. package/bin/skills/astropy/references/time.md +0 -404
  43. package/bin/skills/astropy/references/units.md +0 -178
  44. package/bin/skills/astropy/references/wcs_and_other_modules.md +0 -373
  45. package/bin/skills/audiocraft/SKILL.md +0 -564
  46. package/bin/skills/audiocraft/references/advanced-usage.md +0 -666
  47. package/bin/skills/audiocraft/references/troubleshooting.md +0 -504
  48. package/bin/skills/autogpt/SKILL.md +0 -403
  49. package/bin/skills/autogpt/references/advanced-usage.md +0 -535
  50. package/bin/skills/autogpt/references/troubleshooting.md +0 -420
  51. package/bin/skills/awq/SKILL.md +0 -310
  52. package/bin/skills/awq/references/advanced-usage.md +0 -324
  53. package/bin/skills/awq/references/troubleshooting.md +0 -344
  54. package/bin/skills/axolotl/SKILL.md +0 -158
  55. package/bin/skills/axolotl/references/api.md +0 -5548
  56. package/bin/skills/axolotl/references/dataset-formats.md +0 -1029
  57. package/bin/skills/axolotl/references/index.md +0 -15
  58. package/bin/skills/axolotl/references/other.md +0 -3563
  59. package/bin/skills/benchling-integration/SKILL.md +0 -480
  60. package/bin/skills/benchling-integration/references/api_endpoints.md +0 -883
  61. package/bin/skills/benchling-integration/references/authentication.md +0 -379
  62. package/bin/skills/benchling-integration/references/sdk_reference.md +0 -774
  63. package/bin/skills/bigcode-evaluation-harness/SKILL.md +0 -405
  64. package/bin/skills/bigcode-evaluation-harness/references/benchmarks.md +0 -393
  65. package/bin/skills/bigcode-evaluation-harness/references/custom-tasks.md +0 -424
  66. package/bin/skills/bigcode-evaluation-harness/references/issues.md +0 -394
  67. package/bin/skills/biopython/SKILL.md +0 -443
  68. package/bin/skills/biopython/references/advanced.md +0 -577
  69. package/bin/skills/biopython/references/alignment.md +0 -362
  70. package/bin/skills/biopython/references/blast.md +0 -455
  71. package/bin/skills/biopython/references/databases.md +0 -484
  72. package/bin/skills/biopython/references/phylogenetics.md +0 -566
  73. package/bin/skills/biopython/references/sequence_io.md +0 -285
  74. package/bin/skills/biopython/references/structure.md +0 -564
  75. package/bin/skills/biorxiv-database/SKILL.md +0 -483
  76. package/bin/skills/biorxiv-database/references/api_reference.md +0 -280
  77. package/bin/skills/biorxiv-database/scripts/biorxiv_search.py +0 -445
  78. package/bin/skills/bioservices/SKILL.md +0 -361
  79. package/bin/skills/bioservices/references/identifier_mapping.md +0 -685
  80. package/bin/skills/bioservices/references/services_reference.md +0 -636
  81. package/bin/skills/bioservices/references/workflow_patterns.md +0 -811
  82. package/bin/skills/bioservices/scripts/batch_id_converter.py +0 -347
  83. package/bin/skills/bioservices/scripts/compound_cross_reference.py +0 -378
  84. package/bin/skills/bioservices/scripts/pathway_analysis.py +0 -309
  85. package/bin/skills/bioservices/scripts/protein_analysis_workflow.py +0 -408
  86. package/bin/skills/bitsandbytes/SKILL.md +0 -411
  87. package/bin/skills/bitsandbytes/references/memory-optimization.md +0 -521
  88. package/bin/skills/bitsandbytes/references/qlora-training.md +0 -521
  89. package/bin/skills/bitsandbytes/references/quantization-formats.md +0 -447
  90. package/bin/skills/blip-2/SKILL.md +0 -564
  91. package/bin/skills/blip-2/references/advanced-usage.md +0 -680
  92. package/bin/skills/blip-2/references/troubleshooting.md +0 -526
  93. package/bin/skills/brenda-database/SKILL.md +0 -719
  94. package/bin/skills/brenda-database/references/api_reference.md +0 -537
  95. package/bin/skills/brenda-database/scripts/brenda_queries.py +0 -844
  96. package/bin/skills/brenda-database/scripts/brenda_visualization.py +0 -772
  97. package/bin/skills/brenda-database/scripts/enzyme_pathway_builder.py +0 -1053
  98. package/bin/skills/cellxgene-census/SKILL.md +0 -511
  99. package/bin/skills/cellxgene-census/references/census_schema.md +0 -182
  100. package/bin/skills/cellxgene-census/references/common_patterns.md +0 -351
  101. package/bin/skills/chembl-database/SKILL.md +0 -389
  102. package/bin/skills/chembl-database/references/api_reference.md +0 -272
  103. package/bin/skills/chembl-database/scripts/example_queries.py +0 -278
  104. package/bin/skills/chroma/SKILL.md +0 -406
  105. package/bin/skills/chroma/references/integration.md +0 -38
  106. package/bin/skills/cirq/SKILL.md +0 -346
  107. package/bin/skills/cirq/references/building.md +0 -307
  108. package/bin/skills/cirq/references/experiments.md +0 -572
  109. package/bin/skills/cirq/references/hardware.md +0 -515
  110. package/bin/skills/cirq/references/noise.md +0 -515
  111. package/bin/skills/cirq/references/simulation.md +0 -350
  112. package/bin/skills/cirq/references/transformation.md +0 -416
  113. package/bin/skills/citation-management/SKILL.md +0 -1109
  114. package/bin/skills/citation-management/assets/bibtex_template.bib +0 -264
  115. package/bin/skills/citation-management/assets/citation_checklist.md +0 -386
  116. package/bin/skills/citation-management/references/bibtex_formatting.md +0 -908
  117. package/bin/skills/citation-management/references/citation_validation.md +0 -794
  118. package/bin/skills/citation-management/references/google_scholar_search.md +0 -725
  119. package/bin/skills/citation-management/references/metadata_extraction.md +0 -870
  120. package/bin/skills/citation-management/references/pubmed_search.md +0 -839
  121. package/bin/skills/citation-management/scripts/doi_to_bibtex.py +0 -182
  122. package/bin/skills/citation-management/scripts/extract_metadata.py +0 -570
  123. package/bin/skills/citation-management/scripts/format_bibtex.py +0 -349
  124. package/bin/skills/citation-management/scripts/search_google_scholar.py +0 -251
  125. package/bin/skills/citation-management/scripts/search_pubmed.py +0 -348
  126. package/bin/skills/citation-management/scripts/validate_citations.py +0 -494
  127. package/bin/skills/clinical-decision-support/README.md +0 -129
  128. package/bin/skills/clinical-decision-support/SKILL.md +0 -506
  129. package/bin/skills/clinical-decision-support/assets/biomarker_report_template.tex +0 -380
  130. package/bin/skills/clinical-decision-support/assets/clinical_pathway_template.tex +0 -222
  131. package/bin/skills/clinical-decision-support/assets/cohort_analysis_template.tex +0 -359
  132. package/bin/skills/clinical-decision-support/assets/color_schemes.tex +0 -149
  133. package/bin/skills/clinical-decision-support/assets/example_gbm_cohort.md +0 -208
  134. package/bin/skills/clinical-decision-support/assets/recommendation_strength_guide.md +0 -328
  135. package/bin/skills/clinical-decision-support/assets/treatment_recommendation_template.tex +0 -529
  136. package/bin/skills/clinical-decision-support/references/biomarker_classification.md +0 -719
  137. package/bin/skills/clinical-decision-support/references/clinical_decision_algorithms.md +0 -604
  138. package/bin/skills/clinical-decision-support/references/evidence_synthesis.md +0 -840
  139. package/bin/skills/clinical-decision-support/references/outcome_analysis.md +0 -640
  140. package/bin/skills/clinical-decision-support/references/patient_cohort_analysis.md +0 -427
  141. package/bin/skills/clinical-decision-support/references/treatment_recommendations.md +0 -521
  142. package/bin/skills/clinical-decision-support/scripts/biomarker_classifier.py +0 -383
  143. package/bin/skills/clinical-decision-support/scripts/build_decision_tree.py +0 -417
  144. package/bin/skills/clinical-decision-support/scripts/create_cohort_tables.py +0 -509
  145. package/bin/skills/clinical-decision-support/scripts/generate_survival_analysis.py +0 -441
  146. package/bin/skills/clinical-decision-support/scripts/validate_cds_document.py +0 -326
  147. package/bin/skills/clinical-reports/IMPLEMENTATION_SUMMARY.md +0 -641
  148. package/bin/skills/clinical-reports/README.md +0 -236
  149. package/bin/skills/clinical-reports/SKILL.md +0 -1127
  150. package/bin/skills/clinical-reports/assets/case_report_template.md +0 -352
  151. package/bin/skills/clinical-reports/assets/clinical_trial_csr_template.md +0 -353
  152. package/bin/skills/clinical-reports/assets/clinical_trial_sae_template.md +0 -359
  153. package/bin/skills/clinical-reports/assets/consult_note_template.md +0 -305
  154. package/bin/skills/clinical-reports/assets/discharge_summary_template.md +0 -453
  155. package/bin/skills/clinical-reports/assets/hipaa_compliance_checklist.md +0 -395
  156. package/bin/skills/clinical-reports/assets/history_physical_template.md +0 -305
  157. package/bin/skills/clinical-reports/assets/lab_report_template.md +0 -309
  158. package/bin/skills/clinical-reports/assets/pathology_report_template.md +0 -249
  159. package/bin/skills/clinical-reports/assets/quality_checklist.md +0 -338
  160. package/bin/skills/clinical-reports/assets/radiology_report_template.md +0 -318
  161. package/bin/skills/clinical-reports/assets/soap_note_template.md +0 -253
  162. package/bin/skills/clinical-reports/references/case_report_guidelines.md +0 -570
  163. package/bin/skills/clinical-reports/references/clinical_trial_reporting.md +0 -693
  164. package/bin/skills/clinical-reports/references/data_presentation.md +0 -530
  165. package/bin/skills/clinical-reports/references/diagnostic_reports_standards.md +0 -629
  166. package/bin/skills/clinical-reports/references/medical_terminology.md +0 -588
  167. package/bin/skills/clinical-reports/references/patient_documentation.md +0 -744
  168. package/bin/skills/clinical-reports/references/peer_review_standards.md +0 -585
  169. package/bin/skills/clinical-reports/references/regulatory_compliance.md +0 -577
  170. package/bin/skills/clinical-reports/scripts/check_deidentification.py +0 -332
  171. package/bin/skills/clinical-reports/scripts/compliance_checker.py +0 -78
  172. package/bin/skills/clinical-reports/scripts/extract_clinical_data.py +0 -97
  173. package/bin/skills/clinical-reports/scripts/format_adverse_events.py +0 -97
  174. package/bin/skills/clinical-reports/scripts/generate_report_template.py +0 -149
  175. package/bin/skills/clinical-reports/scripts/terminology_validator.py +0 -126
  176. package/bin/skills/clinical-reports/scripts/validate_case_report.py +0 -323
  177. package/bin/skills/clinical-reports/scripts/validate_trial_report.py +0 -88
  178. package/bin/skills/clinicaltrials-database/SKILL.md +0 -507
  179. package/bin/skills/clinicaltrials-database/references/api_reference.md +0 -358
  180. package/bin/skills/clinicaltrials-database/scripts/query_clinicaltrials.py +0 -215
  181. package/bin/skills/clinpgx-database/SKILL.md +0 -638
  182. package/bin/skills/clinpgx-database/references/api_reference.md +0 -757
  183. package/bin/skills/clinpgx-database/scripts/query_clinpgx.py +0 -518
  184. package/bin/skills/clinvar-database/SKILL.md +0 -362
  185. package/bin/skills/clinvar-database/references/api_reference.md +0 -227
  186. package/bin/skills/clinvar-database/references/clinical_significance.md +0 -218
  187. package/bin/skills/clinvar-database/references/data_formats.md +0 -358
  188. package/bin/skills/clip/SKILL.md +0 -253
  189. package/bin/skills/clip/references/applications.md +0 -207
  190. package/bin/skills/cobrapy/SKILL.md +0 -463
  191. package/bin/skills/cobrapy/references/api_quick_reference.md +0 -655
  192. package/bin/skills/cobrapy/references/workflows.md +0 -593
  193. package/bin/skills/colab-finetuning/SKILL.md +0 -153
  194. package/bin/skills/colab-finetuning/references/bridge-setup.md +0 -68
  195. package/bin/skills/colab-finetuning/references/gpu-tiers.md +0 -54
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  197. package/bin/skills/constitutional-ai/SKILL.md +0 -290
  198. package/bin/skills/cosmic-database/SKILL.md +0 -336
  199. package/bin/skills/cosmic-database/references/cosmic_data_reference.md +0 -220
  200. package/bin/skills/cosmic-database/scripts/download_cosmic.py +0 -231
  201. package/bin/skills/crewai/SKILL.md +0 -498
  202. package/bin/skills/crewai/references/flows.md +0 -438
  203. package/bin/skills/crewai/references/tools.md +0 -429
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  205. package/bin/skills/dask/SKILL.md +0 -456
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  209. package/bin/skills/dask/references/dataframes.md +0 -368
  210. package/bin/skills/dask/references/futures.md +0 -541
  211. package/bin/skills/dask/references/schedulers.md +0 -504
  212. package/bin/skills/datacommons-client/SKILL.md +0 -255
  213. package/bin/skills/datacommons-client/references/getting_started.md +0 -417
  214. package/bin/skills/datacommons-client/references/node.md +0 -250
  215. package/bin/skills/datacommons-client/references/observation.md +0 -185
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  217. package/bin/skills/datamol/SKILL.md +0 -706
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  224. package/bin/skills/deepchem/SKILL.md +0 -597
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  227. package/bin/skills/deepchem/scripts/graph_neural_network.py +0 -338
  228. package/bin/skills/deepchem/scripts/predict_solubility.py +0 -224
  229. package/bin/skills/deepchem/scripts/transfer_learning.py +0 -375
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- # Biomarker Classification and Interpretation Guide
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-
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- ## Overview
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-
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- Biomarkers are measurable indicators of biological state or condition. In clinical decision support, biomarkers guide diagnosis, prognosis, treatment selection, and monitoring. This guide covers genomic, proteomic, and molecular biomarkers with emphasis on clinical actionability.
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-
7
- ## Biomarker Categories
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-
9
- ### Prognostic Biomarkers
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-
11
- **Definition**: Predict clinical outcome (survival, recurrence) regardless of treatment received
12
-
13
- **Examples by Disease**
14
-
15
- **Cancer**
16
- - **Ki-67 index**: High proliferation (>20%) predicts worse outcome in breast cancer
17
- - **TP53 mutation**: Poor prognosis across many cancer types
18
- - **Tumor stage/grade**: TNM staging, histologic grade
19
- - **LDH elevation**: Poor prognosis in melanoma, lymphoma
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- - **AFP elevation**: Poor prognosis in hepatocellular carcinoma
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-
22
- **Cardiovascular**
23
- - **NT-proBNP/BNP**: Elevated levels predict mortality in heart failure
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- - **Troponin**: Predicts adverse events in ACS
25
- - **CRP**: Inflammation marker, predicts cardiovascular events
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-
27
- **Infectious Disease**
28
- - **HIV viral load**: Predicts disease progression if untreated
29
- - **HCV genotype**: Predicts treatment duration needed
30
-
31
- **Application**: Risk stratification, treatment intensity selection, clinical trial enrollment
32
-
33
- ### Predictive Biomarkers
34
-
35
- **Definition**: Identify patients likely to benefit (or not benefit) from specific therapy
36
-
37
- **Positive Predictive Biomarkers (Treatment Benefit)**
38
-
39
- **Oncology - Targeted Therapy**
40
- - **EGFR exon 19 del/L858R → EGFR TKIs**: Response rate 60-70%, PFS 10-14 months
41
- - **ALK rearrangement → ALK inhibitors**: ORR 70-90%, PFS 25-34 months
42
- - **HER2 amplification → Trastuzumab**: Benefit only in HER2+ (IHC 3+ or FISH+)
43
- - **BRAF V600E → BRAF inhibitors**: ORR 50%, PFS 6-7 months (melanoma)
44
- - **PD-L1 ≥50% → Pembrolizumab**: ORR 45%, PFS 10 months vs 6 months (chemo)
45
-
46
- **Oncology - Immunotherapy**
47
- - **MSI-H/dMMR → Anti-PD-1**: ORR 40-60% across tumor types
48
- - **TMB-high → Immunotherapy**: Investigational, some benefit signals
49
- - **PD-L1 expression → Anti-PD-1/PD-L1**: Higher expression correlates with better response
50
-
51
- **Hematology**
52
- - **BCR-ABL → Imatinib (CML)**: Complete cytogenetic response 80%
53
- - **CD20+ → Rituximab (lymphoma)**: Benefit only if CD20-expressing cells
54
- - **CD33+ → Gemtuzumab ozogamicin (AML)**: Benefit in CD33+ subset
55
-
56
- **Negative Predictive Biomarkers (Resistance/No Benefit)**
57
- - **KRAS mutation → Anti-EGFR mAbs (CRC)**: No benefit, contraindicated
58
- - **EGFR T790M → 1st/2nd-gen TKIs**: Resistance mechanism, use osimertinib
59
- - **RAS/RAF wild-type required → BRAF inhibitors (melanoma)**: Paradoxical MAPK activation
60
-
61
- ### Diagnostic Biomarkers
62
-
63
- **Definition**: Detect or confirm presence of disease
64
-
65
- **Infectious Disease**
66
- - **PCR for pathogen DNA/RNA**: SARS-CoV-2, HIV, HCV viral load
67
- - **Antibody titers**: IgM (acute), IgG (prior exposure/immunity)
68
- - **Antigen tests**: Rapid detection (strep, flu, COVID)
69
-
70
- **Autoimmune**
71
- - **ANA**: Screen for lupus, connective tissue disease
72
- - **Anti-CCP**: Specific for rheumatoid arthritis
73
- - **Anti-dsDNA**: Lupus, correlates with disease activity
74
- - **ANCA**: Vasculitis (c-ANCA for GPA, p-ANCA for MPA)
75
-
76
- **Cancer**
77
- - **PSA**: Prostate cancer screening/monitoring
78
- - **CA 19-9**: Pancreatic cancer, biliary obstruction
79
- - **CEA**: Colorectal cancer monitoring
80
- - **AFP**: Hepatocellular carcinoma, germ cell tumors
81
-
82
- ### Pharmacodynamic Biomarkers
83
-
84
- **Definition**: Assess treatment response or mechanism of action
85
-
86
- **Examples**
87
- - **HbA1c**: Glycemic control in diabetes (target <7% typically)
88
- - **LDL cholesterol**: Statin efficacy (target <70 mg/dL in high-risk)
89
- - **Blood pressure**: Antihypertensive efficacy (target <130/80 mmHg)
90
- - **Viral load suppression**: Antiretroviral efficacy (target <20 copies/mL)
91
- - **INR**: Warfarin anticoagulation monitoring (target 2-3 for most indications)
92
-
93
- ## Genomic Biomarkers
94
-
95
- ### Mutation Analysis
96
-
97
- **Driver Mutations (Oncogenic)**
98
- - **Activating mutations**: Constitutive pathway activation (BRAF V600E, EGFR L858R)
99
- - **Inactivating mutations**: Tumor suppressor loss (TP53, PTEN)
100
- - **Hotspot mutations**: Recurrent positions (KRAS G12/G13, PIK3CA H1047R)
101
- - **Variant allele frequency (VAF)**: Clonality (VAF ≈50% clonal, <10% subclonal)
102
-
103
- **Resistance Mutations**
104
- - **EGFR T790M**: Resistance to 1st/2nd-gen TKIs (40-60% of cases)
105
- - **ALK G1202R, I1171N**: Resistance to early ALK inhibitors
106
- - **ESR1 mutations**: Resistance to aromatase inhibitors (breast cancer)
107
- - **RAS mutations**: Acquired resistance to anti-EGFR therapy (CRC)
108
-
109
- **Mutation Detection Methods**
110
- - **Tissue NGS**: Comprehensive genomic profiling, 300-500 genes
111
- - **Liquid biopsy**: ctDNA analysis, non-invasive, serial monitoring
112
- - **PCR-based assays**: Targeted hotspot detection, FDA-approved companion diagnostics
113
- - **Allele-specific PCR**: High sensitivity for known mutations (cobas EGFR test)
114
-
115
- ### Copy Number Variations (CNV)
116
-
117
- **Amplifications**
118
- - **HER2 (ERBB2)**: Breast, gastric cancer → trastuzumab, pertuzumab
119
- - Testing: IHC (0, 1+, 2+, 3+) → FISH if 2+ (HER2/CEP17 ratio ≥2.0)
120
- - **MET amplification**: NSCLC resistance mechanism → crizotinib, capmatinib
121
- - Cut-point: Gene copy number ≥5, GCN/CEP7 ratio ≥2.0
122
- - **EGFR amplification**: Glioblastoma, some NSCLC
123
- - **FGFR2 amplification**: Gastric cancer → investigational FGFR inhibitors
124
-
125
- **Deletions**
126
- - **PTEN loss**: Common in many cancers, predicts PI3K pathway activation
127
- - **RB1 loss**: Small cell transformation, poor prognosis
128
- - **CDKN2A/B deletion**: Cell cycle dysregulation
129
- - **Homozygous deletion**: Complete loss of both alleles (more significant)
130
-
131
- **Detection Methods**
132
- - **FISH (Fluorescence In Situ Hybridization)**: HER2, ALK rearrangements
133
- - **NGS copy number calling**: Depth of coverage analysis
134
- - **SNP array**: Genome-wide CNV detection
135
- - **ddPCR**: Quantitative copy number measurement
136
-
137
- ### Gene Fusions and Rearrangements
138
-
139
- **Oncogenic Fusions**
140
- - **ALK fusions** (NSCLC): EML4-ALK most common (60%), 20+ partners
141
- - Detection: IHC (D5F3 antibody), FISH (break-apart probe), NGS/RNA-seq
142
- - **ROS1 fusions** (NSCLC, glioblastoma): CD74-ROS1, SLC34A2-ROS1, others
143
- - **RET fusions** (NSCLC, thyroid): KIF5B-RET, CCDC6-RET
144
- - **NTRK fusions** (many tumor types, rare): ETV6-NTRK3, others
145
- - Pan-cancer: Larotrectinib, entrectinib approved across tumor types
146
- - **BCR-ABL** (CML, ALL): t(9;22), Philadelphia chromosome
147
-
148
- **Fusion Partner Considerations**
149
- - Partner influences drug sensitivity (EML4-ALK variant 3 more sensitive)
150
- - 5' vs 3' fusion affects detection methods
151
- - Intron breakpoints vary (RNA-seq more comprehensive than DNA panels)
152
-
153
- **Detection Methods**
154
- - **FISH break-apart probes**: ALK, ROS1, RET
155
- - **IHC**: ALK protein overexpression (screening), ROS1
156
- - **RT-PCR**: Targeted fusion detection
157
- - **RNA-seq**: Comprehensive fusion detection, identifies novel partners
158
-
159
- ### Tumor Mutational Burden (TMB)
160
-
161
- **Definition**: Number of somatic mutations per megabase of DNA
162
-
163
- **Classification**
164
- - **TMB-high**: ≥10 mutations/Mb (some definitions ≥20 mut/Mb)
165
- - **TMB-intermediate**: 6-9 mutations/Mb
166
- - **TMB-low**: <6 mutations/Mb
167
-
168
- **Clinical Application**
169
- - **Predictive for immunotherapy**: Higher TMB → more neoantigens → better immune response
170
- - **FDA approval**: Pembrolizumab for TMB-H (≥10 mut/Mb) solid tumors (2020)
171
- - **Limitations**: Not validated in all tumor types, assay variability
172
-
173
- **Tumor Types with Typically High TMB**
174
- - Melanoma (median 10-15 mut/Mb)
175
- - NSCLC (especially smoking-associated, 8-12 mut/Mb)
176
- - Urothelial carcinoma (8-10 mut/Mb)
177
- - Microsatellite instable tumors (30-50 mut/Mb)
178
-
179
- ### Microsatellite Instability (MSI) and Mismatch Repair (MMR)
180
-
181
- **Classification**
182
- - **MSI-high (MSI-H)**: Instability at ≥2 of 5 loci or ≥30% of markers
183
- - **MSI-low (MSI-L)**: Instability at <2 of 5 loci
184
- - **Microsatellite stable (MSS)**: No instability
185
-
186
- **Mismatch Repair Status**
187
- - **dMMR (deficient)**: Loss of MLH1, MSH2, MSH6, or PMS2 by IHC
188
- - **pMMR (proficient)**: Intact expression of all four MMR proteins
189
-
190
- **Clinical Significance**
191
- - **MSI-H/dMMR Tumors**: 3-5% of most solid tumors, 15% of colorectal cancer
192
- - **Immunotherapy Sensitivity**: ORR 30-60% to anti-PD-1 therapy
193
- - Pembrolizumab FDA-approved for MSI-H/dMMR solid tumors (2017)
194
- - Nivolumab ± ipilimumab approved
195
- - **Chemotherapy Resistance**: MSI-H CRC does not benefit from 5-FU adjuvant therapy
196
- - **Lynch Syndrome**: Germline MMR mutation if MSI-H + young age + family history
197
-
198
- **Testing Algorithm**
199
- ```
200
- Colorectal Cancer (all newly diagnosed):
201
- 1. IHC for MMR proteins (MLH1, MSH2, MSH6, PMS2)
202
- ├─ All intact → pMMR (MSS) → Standard chemotherapy if indicated
203
-
204
- └─ Loss of one or more → dMMR (likely MSI-H)
205
- └─ Reflex MLH1 promoter hypermethylation test
206
- ├─ Methylated → Sporadic MSI-H, immunotherapy option
207
- └─ Unmethylated → Germline testing for Lynch syndrome
208
- ```
209
-
210
- ## Expression Biomarkers
211
-
212
- ### Immunohistochemistry (IHC)
213
-
214
- **PD-L1 Expression (Immune Checkpoint)**
215
- - **Assays**: 22C3 (FDA), 28-8, SP263, SP142 (some differences in scoring)
216
- - **Scoring**: Tumor Proportion Score (TPS) = % tumor cells with membrane staining
217
- - TPS <1%: Low/negative
218
- - TPS 1-49%: Intermediate
219
- - TPS ≥50%: High
220
- - **Combined Positive Score (CPS)**: (PD-L1+ tumor + immune cells) / total tumor cells × 100
221
- - Used for some indications (e.g., CPS ≥10 for pembrolizumab in HNSCC)
222
-
223
- **Hormone Receptors (Breast Cancer)**
224
- - **ER/PR Positivity**: ≥1% nuclear staining by IHC (ASCO/CAP guidelines)
225
- - Allred Score 0-8 (proportion + intensity) - historical
226
- - H-score 0-300 (percentage at each intensity) - quantitative
227
- - **Clinical Cut-Points**:
228
- - ER ≥1%: Endocrine therapy indicated
229
- - ER 1-10%: "Low positive," may have lower benefit
230
- - PR loss with ER+: Possible endocrine resistance
231
-
232
- **HER2 Testing (Breast/Gastric Cancer)**
233
- ```
234
- IHC Initial Test:
235
- ├─ 0 or 1+: HER2-negative (no further testing)
236
-
237
- ├─ 2+: Equivocal → Reflex FISH testing
238
- │ ├─ FISH+ (HER2/CEP17 ratio ≥2.0 OR HER2 copies ≥6/cell) → HER2-positive
239
- │ └─ FISH- → HER2-negative
240
-
241
- └─ 3+: HER2-positive (no FISH needed)
242
- └─ Uniform intense complete membrane staining in >10% of tumor cells
243
-
244
- HER2-positive: Trastuzumab-based therapy indicated
245
- HER2-low (IHC 1+ or 2+/FISH-): Trastuzumab deruxtecan eligibility (2022)
246
- ```
247
-
248
- ### RNA Expression Analysis
249
-
250
- **Gene Expression Signatures (Breast Cancer)**
251
-
252
- **Oncotype DX (21-gene assay)**
253
- - **Recurrence Score (RS)**: 0-100
254
- - RS <26: Low risk → Endocrine therapy alone (most patients)
255
- - RS 26-100: High risk → Chemotherapy + endocrine therapy
256
- - **Population**: ER+/HER2-, node-negative or 1-3 positive nodes
257
- - **Evidence**: TAILORx trial (N=10,273) validated RS <26 can omit chemo
258
-
259
- **MammaPrint (70-gene assay)**
260
- - **Result**: High risk vs Low risk (binary)
261
- - **Population**: Early-stage breast cancer, ER+/HER2-
262
- - **Evidence**: MINDACT trial validated low-risk can omit chemo
263
-
264
- **Prosigna (PAM50)**
265
- - **Result**: Risk of Recurrence (ROR) score + intrinsic subtype
266
- - **Subtypes**: Luminal A, Luminal B, HER2-enriched, Basal-like
267
- - **Application**: Post-menopausal, ER+, node-negative or 1-3 nodes
268
-
269
- **RNA-Seq for Fusion Detection**
270
- - **Advantage**: Detects novel fusion partners, quantifies expression
271
- - **Application**: NTRK fusions (rare, many partners), RET fusions
272
- - **Limitation**: Requires fresh/frozen tissue or good-quality FFPE RNA
273
-
274
- ## Molecular Subtypes
275
-
276
- ### Glioblastoma (GBM) Molecular Classification
277
-
278
- **Verhaak 2010 Classification (4 subtypes)**
279
-
280
- **Proneural Subtype**
281
- - **Characteristics**: PDGFRA amplification, IDH1 mutations (secondary GBM), TP53 mutations
282
- - **Age**: Younger patients typically
283
- - **Prognosis**: Better prognosis (median OS 15-18 months)
284
- - **Treatment**: May benefit from bevacizumab less than other subtypes
285
-
286
- **Neural Subtype**
287
- - **Characteristics**: Neuron markers (NEFL, GABRA1, SYT1, SLC12A5)
288
- - **Controversy**: May represent normal brain contamination
289
- - **Prognosis**: Intermediate
290
- - **Treatment**: Standard temozolomide-based therapy
291
-
292
- **Classical Subtype**
293
- - **Characteristics**: EGFR amplification (97%), chromosome 7 gain, chromosome 10 loss
294
- - **Association**: Lacks TP53, PDGFRA, NF1 mutations
295
- - **Prognosis**: Intermediate
296
- - **Treatment**: May benefit from EGFR inhibitors (investigational)
297
-
298
- **Mesenchymal Subtype**
299
- - **Characteristics**: NF1 mutations/deletions, high expression of mesenchymal markers (CHI3L1/YKL-40)
300
- - **Immune Features**: Higher macrophage/microglia infiltration
301
- - **Subgroup**: Mesenchymal-immune-active (high immune signature)
302
- - **Prognosis**: Poor prognosis (median OS 12-13 months)
303
- - **Treatment**: May respond better to anti-angiogenic therapy, immunotherapy investigational
304
-
305
- **Clinical Application**
306
- ```
307
- GBM Molecular Subtyping Report:
308
-
309
- Patient Cohort: Mesenchymal-Immune-Active Subtype (n=15)
310
-
311
- Molecular Features:
312
- - NF1 alterations: 73% (11/15)
313
- - High YKL-40 expression: 100% (15/15)
314
- - Immune gene signature: Elevated (median z-score +2.3)
315
- - CD163+ macrophages: High density (median 180/mm²)
316
-
317
- Treatment Implications:
318
- - Standard therapy: Temozolomide-based (Stupp protocol)
319
- - Consider: Bevacizumab for recurrent disease (may have enhanced benefit)
320
- - Clinical trial: Immune checkpoint inhibitors ± anti-angiogenic therapy
321
- - Prognosis: Median OS 12-14 months (worse than proneural)
322
-
323
- Recommendation:
324
- Enroll in combination immunotherapy trial if eligible, otherwise standard therapy
325
- with early consideration of bevacizumab at progression.
326
- ```
327
-
328
- ### Breast Cancer Intrinsic Subtypes
329
-
330
- **PAM50-Based Classification**
331
-
332
- **Luminal A**
333
- - **Characteristics**: ER+, HER2-, low proliferation (Ki-67 <20%)
334
- - **Gene signature**: High ER-related genes, low proliferation genes
335
- - **Prognosis**: Best prognosis, low recurrence risk
336
- - **Treatment**: Endocrine therapy alone usually sufficient
337
- - **Chemotherapy**: Rarely needed unless high-risk features
338
-
339
- **Luminal B**
340
- - **Characteristics**: ER+, HER2- or HER2+, high proliferation (Ki-67 ≥20%)
341
- - **Subtypes**: Luminal B (HER2-) and Luminal B (HER2+)
342
- - **Prognosis**: Intermediate prognosis
343
- - **Treatment**: Chemotherapy + endocrine therapy; add trastuzumab if HER2+
344
-
345
- **HER2-Enriched**
346
- - **Characteristics**: HER2+, ER-, PR-
347
- - **Gene signature**: High HER2 and proliferation genes, low ER genes
348
- - **Prognosis**: Poor if untreated, good with HER2-targeted therapy
349
- - **Treatment**: Chemotherapy + trastuzumab + pertuzumab
350
-
351
- **Basal-Like**
352
- - **Characteristics**: ER-, PR-, HER2- (triple-negative), high proliferation
353
- - **Gene signature**: Basal cytokeratins (CK5/6, CK17), EGFR
354
- - **Overlap**: 80% concordance with TNBC, but not identical
355
- - **Prognosis**: Aggressive, high early recurrence risk
356
- - **Treatment**: Chemotherapy (platinum, anthracycline), PARP inhibitors if BRCA-mutated
357
- - **Immunotherapy**: PD-L1+ may benefit from pembrolizumab + chemotherapy
358
-
359
- ### Colorectal Cancer Consensus Molecular Subtypes (CMS)
360
-
361
- **CMS1 (14%): MSI Immune**
362
- - **Features**: MSI-high, BRAF mutations, strong immune activation
363
- - **Prognosis**: Poor survival after relapse despite immune infiltration
364
- - **Treatment**: Immunotherapy highly effective, 5-FU chemotherapy ineffective
365
-
366
- **CMS2 (37%): Canonical**
367
- - **Features**: Epithelial, marked WNT and MYC activation
368
- - **Prognosis**: Better survival
369
- - **Treatment**: Benefits from adjuvant chemotherapy
370
-
371
- **CMS3 (13%): Metabolic**
372
- - **Features**: Metabolic dysregulation, KRAS mutations
373
- - **Prognosis**: Intermediate survival
374
- - **Treatment**: May benefit from targeted metabolic therapies (investigational)
375
-
376
- **CMS4 (23%): Mesenchymal**
377
- - **Features**: Stromal infiltration, TGF-β activation, angiogenesis
378
- - **Prognosis**: Worst survival, often diagnosed at advanced stage
379
- - **Treatment**: May benefit from anti-angiogenic therapy (bevacizumab)
380
-
381
- ## Companion Diagnostics
382
-
383
- ### FDA-Approved Biomarker-Drug Pairs
384
-
385
- **Required Testing (Label Indication)**
386
- ```
387
- Biomarker Drug(s) Indication Assay
388
- EGFR exon 19 del/L858R Osimertinib NSCLC cobas EGFR v2, NGS
389
- ALK rearrangement Alectinib, brigatinib NSCLC Vysis ALK FISH, IHC (D5F3)
390
- BRAF V600E Vemurafenib, dabrafenib Melanoma, NSCLC THxID BRAF, cobas BRAF
391
- HER2 amplification Trastuzumab, pertuzumab Breast, gastric HercepTest IHC, FISH
392
- ROS1 rearrangement Crizotinib, entrectinib NSCLC FISH, NGS
393
- PD-L1 ≥50% TPS Pembrolizumab (mono) NSCLC first-line 22C3 pharmDx
394
- MSI-H/dMMR Pembrolizumab Any solid tumor IHC (MMR), PCR (MSI)
395
- NTRK fusion Larotrectinib, entrectinib Pan-cancer FoundationOne CDx
396
- BRCA1/2 mutations Olaparib, talazoparib Breast, ovarian, prostate BRACAnalysis CDx
397
- ```
398
-
399
- ### Complementary Diagnostics (Informative, Not Required)
400
-
401
- - **PD-L1 1-49%**: Informs combination vs monotherapy choice
402
- - **TMB-high**: May predict immunotherapy benefit (not FDA-approved indication)
403
- - **STK11/KEAP1 mutations**: Associated with immunotherapy resistance
404
- - **Homologous recombination deficiency (HRD)**: Predicts PARP inhibitor benefit
405
-
406
- ## Clinical Actionability Frameworks
407
-
408
- ### OncoKB Levels of Evidence (Memorial Sloan Kettering)
409
-
410
- **Level 1: FDA-Approved**
411
- - Biomarker-drug pair with FDA approval in specific tumor type
412
- - Example: EGFR L858R → osimertinib in NSCLC
413
-
414
- **Level 2: Standard Care Off-Label**
415
- - Biomarker-drug in professional guidelines for specific tumor type (not FDA-approved for biomarker)
416
- - Example: BRAF V600E → dabrafenib + trametinib in CRC (NCCN-recommended)
417
-
418
- **Level 3: Clinical Evidence**
419
- - Clinical trial evidence supporting biomarker-drug association
420
- - 3A: Compelling clinical evidence
421
- - 3B: Standard care for different tumor type or investigational
422
-
423
- **Level 4: Biological Evidence**
424
- - Preclinical evidence only (cell lines, mouse models)
425
- - 4: Biological evidence supporting association
426
-
427
- **Level R1-R2: Resistance**
428
- - R1: Standard care associated with resistance
429
- - R2: Investigational or preclinical resistance evidence
430
-
431
- ### CIViC (Clinical Interpretation of Variants in Cancer)
432
-
433
- **Evidence Levels**
434
- - **A**: Validated in clinical practice or validated by regulatory association
435
- - **B**: Clinical trial or other primary patient data supporting association
436
- - **C**: Case study with molecular analysis
437
- - **D**: Preclinical evidence (cell culture, animal models)
438
- - **E**: Inferential association (literature review, expert opinion)
439
-
440
- **Clinical Significance Tiers**
441
- - **Tier I**: Variants with strong clinical significance (predictive, diagnostic, prognostic in professional guidelines)
442
- - **Tier II**: Variants with potential clinical significance (clinical trial or case study evidence)
443
- - **Tier III**: Variants with uncertain significance
444
- - **Tier IV**: Benign or likely benign variants
445
-
446
- ## Multi-Biomarker Panels
447
-
448
- ### Comprehensive Genomic Profiling (CGP)
449
-
450
- **FoundationOne CDx**
451
- - **Genes**: 324 genes (SNVs, indels, CNVs, rearrangements)
452
- - **Additional**: TMB, MSI status
453
- - **FDA-Approved**: Companion diagnostic for 18+ targeted therapies
454
- - **Turnaround**: 10-14 days
455
- - **Tissue**: FFPE, 40 unstained slides or tissue block
456
-
457
- **Guardant360 CDx (Liquid Biopsy)**
458
- - **Genes**: 74 genes in cell-free DNA (cfDNA)
459
- - **Sample**: 2 tubes of blood (20 mL total)
460
- - **FDA-Approved**: Companion diagnostic for osimertinib (EGFR), NSCLC
461
- - **Application**: Non-invasive, serial monitoring, when tissue unavailable
462
- - **Limitation**: Lower sensitivity than tissue (especially for low tumor burden)
463
-
464
- **Tempus xT**
465
- - **Genes**: 648 genes (DNA) + whole transcriptome (RNA)
466
- - **Advantage**: RNA detects fusions, expression signatures
467
- - **Application**: Research and clinical use
468
- - **Not FDA-Approved**: Not a companion diagnostic currently
469
-
470
- ### Testing Recommendations by Tumor Type
471
-
472
- **NSCLC (NCCN Guidelines)**
473
- ```
474
- Broad molecular profiling for all advanced NSCLC at diagnosis:
475
-
476
- Required (FDA-approved therapies available):
477
- ✓ EGFR mutations (exons 18, 19, 20, 21)
478
- ✓ ALK rearrangement
479
- ✓ ROS1 rearrangement
480
- ✓ BRAF V600E
481
- ✓ MET exon 14 skipping
482
- ✓ RET rearrangements
483
- ✓ NTRK fusions
484
- ✓ KRAS G12C
485
- ✓ PD-L1 IHC
486
-
487
- Recommended (to inform treatment strategy):
488
- ✓ Comprehensive NGS panel (captures all above + emerging targets)
489
- ✓ Consider liquid biopsy if tissue insufficient
490
-
491
- At progression on targeted therapy:
492
- ✓ Repeat tissue biopsy or liquid biopsy for resistance mechanisms
493
- ✓ Examples: EGFR T790M, ALK resistance mutations, MET amplification
494
- ```
495
-
496
- **Metastatic Colorectal Cancer**
497
- ```
498
- Required before anti-EGFR therapy (cetuximab, panitumumab):
499
- ✓ RAS testing (KRAS exons 2, 3, 4; NRAS exons 2, 3, 4)
500
- └─ RAS mutation → Do NOT use anti-EGFR therapy (resistance)
501
- ✓ BRAF V600E
502
- └─ If BRAF V600E+ → Consider encorafenib + cetuximab + binimetinib
503
-
504
- Recommended for all metastatic CRC:
505
- ✓ MSI/MMR testing (immunotherapy indication)
506
- ✓ HER2 amplification (investigational trastuzumab-based therapy if RAS/BRAF WT)
507
- ✓ NTRK fusions (rare, <1%, but actionable)
508
-
509
- Left-sided vs Right-sided:
510
- - Left-sided (descending, sigmoid, rectum): Better prognosis, anti-EGFR more effective
511
- - Right-sided (cecum, ascending): Worse prognosis, anti-EGFR less effective, consider bevacizumab
512
- ```
513
-
514
- **Melanoma**
515
- ```
516
- All advanced melanoma:
517
- ✓ BRAF V600 mutation (30-50% of cutaneous melanoma)
518
- └─ If BRAF V600E/K → Dabrafenib + trametinib or vemurafenib + cobimetinib
519
- ✓ NRAS mutation (20-30%)
520
- └─ No targeted therapy approved, consider MEK inhibitor trials
521
- ✓ KIT mutations (mucosal, acral, chronic sun-damaged melanoma)
522
- └─ If KIT exon 11 or 13 mutation → Imatinib (off-label)
523
- ✓ PD-L1 (optional, not required for immunotherapy eligibility)
524
-
525
- Note: Uveal melanoma has different biology (GNAQ, GNA11 mutations)
526
- ```
527
-
528
- ## Biomarker Cut-Points and Thresholds
529
-
530
- ### Establishing Clinical Cut-Points
531
-
532
- **Methods for Cut-Point Determination**
533
-
534
- **Data-Driven Approaches**
535
- - **Median split**: Simple but arbitrary, may not be optimal
536
- - **Tertiles/quartiles**: Categorizes into 3-4 groups
537
- - **ROC curve analysis**: Maximizes sensitivity and specificity
538
- - **Maximally selected rank statistics**: Finds optimal prognostic cut-point
539
- - **Validation required**: Independent cohort confirmation essential
540
-
541
- **Biologically Informed**
542
- - **Detection limit**: Assay lower limit of quantification
543
- - **Mechanism-based**: Threshold for pathway activation
544
- - **Pharmacodynamic**: Threshold for target engagement
545
- - **Normal range**: Comparison to healthy individuals
546
-
547
- **Clinically Defined**
548
- - **Guideline-recommended**: Established by professional societies
549
- - **Regulatory-approved**: FDA-specified threshold for companion diagnostic
550
- - **Trial-defined**: Cut-point used in pivotal clinical trial
551
-
552
- **PD-L1 Example**
553
- - **Cut-points**: 1%, 5%, 10%, 50% TPS used in different trials
554
- - **Context-dependent**: Varies by drug, disease, line of therapy
555
- - **≥50%**: Pembrolizumab monotherapy (KEYNOTE-024)
556
- - **≥1%**: Atezolizumab combinations, broader population
557
-
558
- ### Continuous vs Categorical
559
-
560
- **Continuous Analysis Advantages**
561
- - Preserves information (no dichotomization loss)
562
- - Statistical power maintained
563
- - Can assess dose-response relationship
564
- - HR per unit increase or per standard deviation
565
-
566
- **Categorical Analysis Advantages**
567
- - Clinically interpretable (high vs low)
568
- - Facilitates treatment decisions (binary: use targeted therapy yes/no)
569
- - Aligns with regulatory approvals (biomarker-positive = eligible)
570
-
571
- **Best Practice**: Report both continuous and categorical analyses
572
- - Cox model with continuous biomarker
573
- - Stratified analysis by clinically relevant cut-point
574
- - Subgroup analysis to confirm consistency
575
-
576
- ## Germline vs Somatic Testing
577
-
578
- ### Germline (Inherited) Mutations
579
-
580
- **Indications for Germline Testing**
581
- - **Cancer predisposition syndromes**: BRCA1/2, Lynch syndrome (MLH1, MSH2), Li-Fraumeni (TP53)
582
- - **Family history**: Multiple affected relatives, young age at diagnosis
583
- - **Tumor features**: MSI-H in young patient, triple-negative breast cancer <60 years
584
- - **Treatment implications**: PARP inhibitors for BRCA-mutated (germline or somatic)
585
-
586
- **Common Hereditary Cancer Syndromes**
587
- - **BRCA1/2**: Breast, ovarian, pancreatic, prostate cancer
588
- - Testing: All ovarian cancer, TNBC <60 years, male breast cancer
589
- - Treatment: PARP inhibitors (olaparib, talazoparib)
590
- - Prevention: Prophylactic mastectomy, oophorectomy (risk-reducing)
591
- - **Lynch syndrome (MLH1, MSH2, MSH6, PMS2)**: Colorectal, endometrial, ovarian, gastric
592
- - Testing: MSI-H/dMMR tumors, Amsterdam II criteria families
593
- - Surveillance: Colonoscopy every 1-2 years starting age 20-25
594
- - **Li-Fraumeni (TP53)**: Diverse cancers at young age
595
- - **PTEN (Cowden syndrome)**: Breast, thyroid, endometrial cancer
596
-
597
- **Genetic Counseling**
598
- - Pre-test counseling: Implications for patient and family
599
- - Post-test counseling: Management, surveillance, family testing
600
- - Informed consent: Genetic discrimination concerns (GINA protections)
601
-
602
- ### Somatic (Tumor-Only) Testing
603
-
604
- **Tumor Tissue Testing**
605
- - Detects mutations present in cancer cells only (not inherited)
606
- - Most cancer driver mutations are somatic (KRAS, EGFR in lung cancer)
607
- - No implications for family members
608
- - Guides therapy selection
609
-
610
- **Distinguishing Germline from Somatic**
611
- - **Variant allele frequency**: Germline ~50% (heterozygous) or ~100% (homozygous); somatic variable
612
- - **Matched normal**: Paired tumor-normal sequencing definitive
613
- - **Databases**: Germline variant databases (gnomAD, ClinVar)
614
- - **Reflex germline testing**: Trigger testing if pathogenic germline variant suspected
615
-
616
- ## Reporting Biomarker Results
617
-
618
- ### Structured Report Template
619
-
620
- ```
621
- MOLECULAR PROFILING REPORT
622
-
623
- Patient: [De-identified ID]
624
- Tumor Type: Non-Small Cell Lung Adenocarcinoma
625
- Specimen: Lung biopsy (left upper lobe)
626
- Testing Date: [Date]
627
- Report Date: [Date]
628
-
629
- METHODOLOGY
630
- - Assay: FoundationOne CDx (comprehensive genomic profiling)
631
- - Specimen Type: Formalin-fixed paraffin-embedded (FFPE)
632
- - Tumor Content: 40% (adequate for testing)
633
-
634
- RESULTS SUMMARY
635
- Biomarkers Detected: 4
636
- - 1 FDA-approved therapy target
637
- - 1 prognostic biomarker
638
- - 2 variants of uncertain significance
639
-
640
- ACTIONABLE FINDINGS
641
-
642
- Tier 1: FDA-Approved Targeted Therapy Available
643
- ━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━
644
- EGFR Exon 19 Deletion (p.E746_A750del)
645
- Variant Allele Frequency: 42%
646
- Clinical Significance: Sensitizing mutation
647
- FDA-Approved Therapy: Osimertinib (Tagrisso) 80 mg daily
648
- Evidence: FLAURA trial - median PFS 18.9 vs 10.2 months (HR 0.46, p<0.001)
649
- Guideline: NCCN Category 1 preferred first-line
650
- Recommendation: Strong recommendation for EGFR TKI therapy (GRADE 1A)
651
-
652
- Tier 2: Prognostic Biomarker
653
- ━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━━
654
- TP53 Mutation (p.R273H)
655
- Variant Allele Frequency: 85%
656
- Clinical Significance: Poor prognostic marker, no targeted therapy
657
- Implication: Associated with worse survival, does not impact first-line treatment selection
658
-
659
- BIOMARKERS ASSESSED - NEGATIVE
660
- - ALK rearrangement: Not detected
661
- - ROS1 rearrangement: Not detected
662
- - BRAF V600E: Not detected
663
- - MET exon 14 skipping: Not detected
664
- - RET rearrangement: Not detected
665
- - KRAS mutation: Not detected
666
- - PD-L1 IHC: Separate report (TPS 30%)
667
-
668
- TUMOR MUTATIONAL BURDEN: 8 mutations/Mb (Intermediate)
669
- - Interpretation: Below threshold for TMB-high designation (≥10 mut/Mb)
670
- - Clinical relevance: May still benefit from immunotherapy combinations
671
-
672
- MICROSATELLITE STATUS: Stable (MSS)
673
-
674
- CLINICAL RECOMMENDATIONS
675
-
676
- Primary Recommendation:
677
- First-line therapy with osimertinib 80 mg PO daily until progression or unacceptable toxicity.
678
-
679
- Monitoring:
680
- - CT imaging every 6 weeks for first 12 weeks, then every 9 weeks
681
- - At progression, repeat tissue or liquid biopsy for resistance mechanisms (T790M, C797S, MET amplification)
682
-
683
- Alternative Options:
684
- - Clinical trial enrollment for novel EGFR TKI combinations
685
- - Erlotinib or afatinib (second-line for osimertinib if used first-line)
686
-
687
- References:
688
- 1. Soria JC, et al. Osimertinib in Untreated EGFR-Mutated Advanced NSCLC. NEJM 2018.
689
- 2. NCCN Guidelines for Non-Small Cell Lung Cancer v4.2024.
690
-
691
- Report Prepared By: [Lab Name]
692
- Medical Director: [Name, MD, PhD]
693
- CLIA #: [Number] | CAP #: [Number]
694
- ```
695
-
696
- ## Quality Assurance
697
-
698
- ### Analytical Validation
699
-
700
- - **Sensitivity**: Minimum 5-10% variant allele frequency detection
701
- - **Specificity**: <1% false positive rate
702
- - **Reproducibility**: >95% concordance between replicates
703
- - **Accuracy**: >99% concordance with validated orthogonal method
704
- - **Turnaround time**: Median time from sample receipt to report
705
-
706
- ### Clinical Validation
707
-
708
- - **Positive Predictive Value**: % biomarker+ patients who respond to therapy
709
- - **Negative Predictive Value**: % biomarker- patients who do not respond
710
- - **Clinical Utility**: Does testing improve patient outcomes?
711
- - **Cost-Effectiveness**: QALY gained vs cost of testing and treatment
712
-
713
- ### Proficiency Testing
714
-
715
- - CAP/CLIA proficiency testing for clinical labs
716
- - Participate in external quality assurance schemes
717
- - Blinded sample exchange with reference laboratories
718
- - Document corrective actions for failures
719
-