@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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- # Patient Cohort Analysis Guide
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-
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- ## Overview
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-
5
- Patient cohort analysis involves systematically studying groups of patients to identify patterns, compare outcomes, and derive clinical insights. In pharmaceutical and clinical research settings, cohort analysis is essential for understanding treatment effectiveness, biomarker correlations, and patient stratification.
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-
7
- ## Patient Stratification Methods
8
-
9
- ### Biomarker-Based Stratification
10
-
11
- **Genomic Biomarkers**
12
- - **Mutations**: Driver mutations (EGFR, KRAS, BRAF), resistance mutations (T790M)
13
- - **Copy Number Variations**: Amplifications (HER2, MET), deletions (PTEN, RB1)
14
- - **Gene Fusions**: ALK, ROS1, NTRK, RET rearrangements
15
- - **Tumor Mutational Burden (TMB)**: High (≥10 mut/Mb) vs low TMB
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- - **Microsatellite Instability**: MSI-high vs MSS/MSI-low
17
-
18
- **Expression Biomarkers**
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- - **IHC Scores**: PD-L1 TPS (<1%, 1-49%, ≥50%), HER2 (0, 1+, 2+, 3+)
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- - **RNA Expression**: Gene signatures, pathway activity scores
21
- - **Protein Levels**: Ki-67 proliferation index, hormone receptors (ER/PR)
22
-
23
- **Molecular Subtypes**
24
- - **Breast Cancer**: Luminal A, Luminal B, HER2-enriched, Triple-negative
25
- - **Glioblastoma**: Proneural, neural, classical, mesenchymal
26
- - **Lung Adenocarcinoma**: Terminal respiratory unit, proximal inflammatory, proximal proliferative
27
- - **Colorectal Cancer**: CMS1-4 (consensus molecular subtypes)
28
-
29
- ### Demographic Stratification
30
-
31
- - **Age Groups**: Pediatric (<18), young adult (18-39), middle-age (40-64), elderly (65-79), very elderly (≥80)
32
- - **Sex/Gender**: Male, female, sex-specific biomarkers
33
- - **Race/Ethnicity**: FDA-recognized categories, ancestry-informative markers
34
- - **Geographic Location**: Regional variation in disease prevalence
35
-
36
- ### Clinical Stratification
37
-
38
- **Disease Characteristics**
39
- - **Stage**: TNM staging (I, II, III, IV), Ann Arbor (lymphoma)
40
- - **Grade**: Well-differentiated (G1), moderately differentiated (G2), poorly differentiated (G3), undifferentiated (G4)
41
- - **Histology**: Adenocarcinoma vs squamous vs other subtypes
42
- - **Disease Burden**: Tumor volume, number of lesions, organ involvement
43
-
44
- **Patient Status**
45
- - **Performance Status**: ECOG (0-4), Karnofsky (0-100)
46
- - **Comorbidities**: Charlson Comorbidity Index, organ dysfunction
47
- - **Prior Treatment**: Treatment-naïve, previously treated, lines of therapy
48
- - **Response to Prior Therapy**: Responders vs non-responders, progressive disease
49
-
50
- ### Risk Stratification
51
-
52
- **Prognostic Scores**
53
- - **Cancer**: AJCC staging, Gleason score, Nottingham grade
54
- - **Cardiovascular**: Framingham risk, TIMI, GRACE, CHADS2-VASc
55
- - **Liver Disease**: Child-Pugh class, MELD score
56
- - **Renal Disease**: eGFR categories, albuminuria stages
57
-
58
- **Composite Risk Models**
59
- - Low risk: Good prognosis, less aggressive treatment
60
- - Intermediate risk: Moderate prognosis, standard treatment
61
- - High risk: Poor prognosis, intensive treatment or clinical trials
62
-
63
- ## Cluster Analysis and Subgroup Identification
64
-
65
- ### Unsupervised Clustering
66
-
67
- **Methods**
68
- - **K-means**: Partition-based clustering with pre-defined number of clusters
69
- - **Hierarchical Clustering**: Agglomerative or divisive, creates dendrogram
70
- - **DBSCAN**: Density-based clustering, identifies outliers
71
- - **Consensus Clustering**: Robust cluster identification across multiple runs
72
-
73
- **Applications**
74
- - Molecular subtype discovery (e.g., GBM mesenchymal-immune-active cluster)
75
- - Patient phenotype identification
76
- - Treatment response patterns
77
- - Multi-omic data integration
78
-
79
- ### Supervised Classification
80
-
81
- **Approaches**
82
- - **Pre-defined Criteria**: Clinical guidelines, established biomarker cut-points
83
- - **Machine Learning**: Random forests, support vector machines for prediction
84
- - **Neural Networks**: Deep learning for complex pattern recognition
85
- - **Validated Signatures**: Published gene expression panels (Oncotype DX, MammaPrint)
86
-
87
- ### Validation Requirements
88
-
89
- - **Internal Validation**: Cross-validation, bootstrap resampling
90
- - **External Validation**: Independent cohort confirmation
91
- - **Clinical Validation**: Prospective trial confirmation of utility
92
- - **Analytical Validation**: Assay reproducibility, inter-lab concordance
93
-
94
- ## Outcome Metrics
95
-
96
- ### Survival Endpoints
97
-
98
- **Overall Survival (OS)**
99
- - Definition: Time from treatment start (or randomization) to death from any cause
100
- - Censoring: Last known alive date for patients lost to follow-up
101
- - Reporting: Median OS, 1-year/2-year/5-year OS rates, hazard ratio
102
- - Gold Standard: Primary endpoint for regulatory approval
103
-
104
- **Progression-Free Survival (PFS)**
105
- - Definition: Time from treatment start to disease progression or death
106
- - Assessment: RECIST v1.1, iRECIST (for immunotherapy)
107
- - Advantages: Earlier readout than OS, direct measure of treatment benefit
108
- - Limitations: Requires imaging, subject to assessment timing
109
-
110
- **Disease-Free Survival (DFS)**
111
- - Definition: Time from complete response to recurrence or death (adjuvant setting)
112
- - Application: Post-surgery, post-curative treatment
113
- - Synonyms: Recurrence-free survival (RFS), event-free survival (EFS)
114
-
115
- ### Response Endpoints
116
-
117
- **Objective Response Rate (ORR)**
118
- - Definition: Proportion achieving complete response (CR) or partial response (PR)
119
- - Measurement: RECIST v1.1 criteria (≥30% tumor shrinkage for PR)
120
- - Reporting: ORR with 95% confidence interval
121
- - Advantage: Earlier endpoint than survival
122
-
123
- **Duration of Response (DOR)**
124
- - Definition: Time from first response (CR/PR) to progression
125
- - Population: Responders only
126
- - Clinical Relevance: Durability of treatment benefit
127
- - Reporting: Median DOR among responders
128
-
129
- **Disease Control Rate (DCR)**
130
- - Definition: CR + PR + stable disease (SD)
131
- - Threshold: SD must persist ≥6-8 weeks typically
132
- - Application: Less stringent than ORR, captures clinical benefit
133
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134
- ### Quality of Life and Functional Status
135
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136
- **Performance Status**
137
- - **ECOG Scale**: 0 (fully active) to 4 (bedridden)
138
- - **Karnofsky Scale**: 100% (normal) to 0% (dead)
139
- - **Assessment Frequency**: Baseline and each cycle
140
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141
- **Patient-Reported Outcomes (PROs)**
142
- - **Symptom Scales**: EORTC QLQ-C30, FACT-G
143
- - **Disease-Specific**: FACT-L (lung), FACT-B (breast)
144
- - **Toxicity**: PRO-CTCAE for adverse events
145
- - **Reporting**: Change from baseline, clinically meaningful differences
146
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147
- ### Safety and Tolerability
148
-
149
- **Adverse Events (AEs)**
150
- - **Grading**: CTCAE v5.0 (Grade 1-5)
151
- - **Attribution**: Related vs unrelated to treatment
152
- - **Serious AEs (SAEs)**: Death, life-threatening, hospitalization, disability
153
- - **Reporting**: Incidence, severity, time to onset, resolution
154
-
155
- **Treatment Modifications**
156
- - **Dose Reductions**: Proportion requiring dose decrease
157
- - **Dose Delays**: Treatment interruptions, cycle delays
158
- - **Discontinuations**: Treatment termination due to toxicity
159
- - **Relative Dose Intensity**: Actual dose / planned dose ratio
160
-
161
- ## Statistical Methods for Group Comparisons
162
-
163
- ### Continuous Variables
164
-
165
- **Parametric Tests (Normal Distribution)**
166
- - **Two Groups**: Independent t-test, paired t-test
167
- - **Multiple Groups**: ANOVA (analysis of variance), repeated measures ANOVA
168
- - **Reporting**: Mean ± SD, mean difference with 95% CI, p-value
169
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170
- **Non-Parametric Tests (Non-Normal Distribution)**
171
- - **Two Groups**: Mann-Whitney U test (Wilcoxon rank-sum)
172
- - **Paired Data**: Wilcoxon signed-rank test
173
- - **Multiple Groups**: Kruskal-Wallis test
174
- - **Reporting**: Median [IQR], median difference, p-value
175
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176
- ### Categorical Variables
177
-
178
- **Chi-Square Test**
179
- - **Application**: Compare proportions between ≥2 groups
180
- - **Assumptions**: Expected count ≥5 in each cell
181
- - **Reporting**: Proportions, chi-square statistic, df, p-value
182
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183
- **Fisher's Exact Test**
184
- - **Application**: 2x2 tables with small sample sizes (expected count <5)
185
- - **Advantage**: Exact p-value, no large-sample approximation
186
- - **Limitation**: Computationally intensive for large tables
187
-
188
- ### Survival Analysis
189
-
190
- **Kaplan-Meier Method**
191
- - **Application**: Estimate survival curves with censored data
192
- - **Output**: Survival probability at each time point, median survival
193
- - **Visualization**: Step function curves with 95% CI bands
194
-
195
- **Log-Rank Test**
196
- - **Application**: Compare survival curves between groups
197
- - **Null Hypothesis**: No difference in survival distributions
198
- - **Reporting**: Chi-square statistic, df, p-value
199
- - **Limitation**: Assumes proportional hazards
200
-
201
- **Cox Proportional Hazards Model**
202
- - **Application**: Multivariable survival analysis
203
- - **Output**: Hazard ratio (HR) with 95% CI for each covariate
204
- - **Interpretation**: HR > 1 (increased risk), HR < 1 (decreased risk)
205
- - **Assumptions**: Proportional hazards (test with Schoenfeld residuals)
206
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207
- ### Effect Sizes
208
-
209
- **Hazard Ratio (HR)**
210
- - Definition: Ratio of hazard rates between groups
211
- - Interpretation: HR = 0.5 means 50% reduction in risk
212
- - Reporting: HR (95% CI), p-value
213
- - Example: HR = 0.65 (0.52-0.81), p<0.001
214
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215
- **Odds Ratio (OR)**
216
- - Application: Case-control studies, logistic regression
217
- - Interpretation: OR > 1 (increased odds), OR < 1 (decreased odds)
218
- - Reporting: OR (95% CI), p-value
219
-
220
- **Risk Ratio (RR) / Relative Risk**
221
- - Application: Cohort studies, clinical trials
222
- - Interpretation: RR = 2.0 means 2-fold increased risk
223
- - More intuitive than OR for interpreting probabilities
224
-
225
- ### Multiple Testing Corrections
226
-
227
- **Bonferroni Correction**
228
- - Method: Divide α by number of tests (α/n)
229
- - Example: 5 tests → significance threshold = 0.05/5 = 0.01
230
- - Conservative: Reduces Type I error but increases Type II error
231
-
232
- **False Discovery Rate (FDR)**
233
- - Method: Benjamini-Hochberg procedure
234
- - Interpretation: Expected proportion of false positives among significant results
235
- - Less Conservative: More power than Bonferroni
236
-
237
- **Family-Wise Error Rate (FWER)**
238
- - Method: Control probability of any false positive
239
- - Application: When even one false positive is problematic
240
- - Examples: Bonferroni, Holm-Bonferroni
241
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242
- ## Biomarker Correlation with Outcomes
243
-
244
- ### Predictive Biomarkers
245
-
246
- **Definition**: Biomarkers that identify patients likely to respond to a specific treatment
247
-
248
- **Examples**
249
- - **PD-L1 ≥50%**: Predicts response to pembrolizumab monotherapy (NSCLC)
250
- - **HER2 3+**: Predicts response to trastuzumab (breast cancer)
251
- - **EGFR mutations**: Predicts response to EGFR TKIs (lung cancer)
252
- - **BRAF V600E**: Predicts response to vemurafenib (melanoma)
253
- - **MSI-H/dMMR**: Predicts response to immune checkpoint inhibitors
254
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255
- **Analysis**
256
- - Stratified analysis: Compare treatment effect within biomarker-positive vs negative
257
- - Interaction test: Test if treatment effect differs by biomarker status
258
- - Reporting: HR in biomarker+ vs biomarker-, interaction p-value
259
-
260
- ### Prognostic Biomarkers
261
-
262
- **Definition**: Biomarkers that predict outcome regardless of treatment
263
-
264
- **Examples**
265
- - **High Ki-67**: Poor prognosis independent of treatment (breast cancer)
266
- - **TP53 mutation**: Poor prognosis in many cancers
267
- - **Low albumin**: Poor prognosis marker (many diseases)
268
- - **Elevated LDH**: Poor prognosis (melanoma, lymphoma)
269
-
270
- **Analysis**
271
- - Compare outcomes across biomarker levels in untreated or uniformly treated cohort
272
- - Multivariable Cox model adjusting for other prognostic factors
273
- - Validate in independent cohorts
274
-
275
- ### Continuous Biomarker Analysis
276
-
277
- **Cut-Point Selection**
278
- - **Data-Driven**: Maximally selected rank statistics, ROC curve analysis
279
- - **Literature-Based**: Established clinical cut-points
280
- - **Median/Tertiles**: Simple divisions for exploration
281
- - **Validation**: Cut-points must be validated in independent cohort
282
-
283
- **Continuous Analysis**
284
- - Treat biomarker as continuous variable in Cox model
285
- - Report HR per unit increase or per standard deviation
286
- - Spline curves to assess non-linear relationships
287
- - Advantage: No information loss from dichotomization
288
-
289
- ## Data Presentation
290
-
291
- ### Baseline Characteristics Table (Table 1)
292
-
293
- **Standard Format**
294
- ```
295
- Characteristic Group A (n=50) Group B (n=45) p-value
296
- Age, years (median [IQR]) 62 [54-68] 59 [52-66] 0.34
297
- Sex, n (%)
298
- Male 30 (60%) 28 (62%) 0.82
299
- Female 20 (40%) 17 (38%)
300
- ECOG PS, n (%)
301
- 0-1 42 (84%) 39 (87%) 0.71
302
- 2 8 (16%) 6 (13%)
303
- Biomarker+, n (%) 23 (46%) 21 (47%) 0.94
304
- ```
305
-
306
- **Key Principles**
307
- - Report all clinically relevant baseline variables
308
- - Use appropriate summary statistics (mean±SD for normal, median[IQR] for skewed)
309
- - Include sample size for each group
310
- - Report p-values for group comparisons (but baseline imbalances expected by chance)
311
- - Do NOT adjust baseline p-values for multiple testing
312
-
313
- ### Efficacy Outcomes Table
314
-
315
- **Response Outcomes**
316
- ```
317
- Outcome Group A (n=50) Group B (n=45) p-value
318
- ORR, n (%) [95% CI] 25 (50%) [36-64] 15 (33%) [20-48] 0.08
319
- Complete Response 3 (6%) 1 (2%)
320
- Partial Response 22 (44%) 14 (31%)
321
- DCR, n (%) [95% CI] 40 (80%) [66-90] 35 (78%) [63-89] 0.79
322
- Median DOR, months (95% CI) 8.2 (6.1-11.3) 6.8 (4.9-9.7) 0.12
323
- ```
324
-
325
- **Survival Outcomes**
326
- ```
327
- Endpoint Group A Group B HR (95% CI) p-value
328
- Median PFS, months (95% CI) 10.2 (8.3-12.1) 6.5 (5.1-7.9) 0.62 (0.41-0.94) 0.02
329
- 12-month PFS rate 42% 28%
330
- Median OS, months (95% CI) 21.3 (17.8-NR) 15.7 (12.4-19.1) 0.71 (0.45-1.12) 0.14
331
- 12-month OS rate 68% 58%
332
- ```
333
-
334
- ### Safety and Tolerability Table
335
-
336
- **Adverse Events**
337
- ```
338
- Adverse Event Any Grade, n (%) Grade 3-4, n (%)
339
- Group A Group B Group A Group B
340
- Fatigue 35 (70%) 32 (71%) 3 (6%) 2 (4%)
341
- Nausea 28 (56%) 25 (56%) 1 (2%) 1 (2%)
342
- Neutropenia 15 (30%) 18 (40%) 8 (16%) 10 (22%)
343
- Thrombocytopenia 12 (24%) 14 (31%) 4 (8%) 6 (13%)
344
- Hepatotoxicity 8 (16%) 6 (13%) 2 (4%) 1 (2%)
345
- Treatment discontinuation 6 (12%) 8 (18%) - -
346
- ```
347
-
348
- ### Visualization Formats
349
-
350
- **Survival Curves**
351
- - Kaplan-Meier plots with 95% CI bands
352
- - Number at risk table below x-axis
353
- - Log-rank p-value and HR prominently displayed
354
- - Clear legend identifying groups
355
-
356
- **Forest Plots**
357
- - Subgroup analysis showing HR with 95% CI for each subgroup
358
- - Test for interaction assessing heterogeneity
359
- - Overall effect at bottom
360
-
361
- **Waterfall Plots**
362
- - Individual patient best response (% change from baseline)
363
- - Ordered from best to worst response
364
- - Color-coded by response category (CR, PR, SD, PD)
365
- - Biomarker status annotation
366
-
367
- **Swimmer Plots**
368
- - Time on treatment for each patient
369
- - Response duration for responders
370
- - Treatment modifications marked
371
- - Ongoing treatments indicated with arrow
372
-
373
- ## Quality Control and Validation
374
-
375
- ### Data Quality Checks
376
-
377
- - **Completeness**: Missing data patterns, loss to follow-up
378
- - **Consistency**: Cross-field validation, logical checks
379
- - **Outliers**: Identify and investigate extreme values
380
- - **Duplicates**: Patient ID verification, enrollment checks
381
-
382
- ### Statistical Assumptions
383
-
384
- - **Normality**: Shapiro-Wilk test, Q-Q plots for continuous variables
385
- - **Proportional Hazards**: Schoenfeld residuals for Cox models
386
- - **Independence**: Check for clustering, matched data
387
- - **Missing Data**: Assess mechanism (MCAR, MAR, NMAR), handle appropriately
388
-
389
- ### Reporting Standards
390
-
391
- - **CONSORT**: Randomized controlled trials
392
- - **STROBE**: Observational studies
393
- - **REMARK**: Tumor marker prognostic studies
394
- - **STARD**: Diagnostic accuracy studies
395
- - **TRIPOD**: Prediction model development/validation
396
-
397
- ## Clinical Interpretation
398
-
399
- ### Translating Statistics to Clinical Meaning
400
-
401
- **Statistical Significance vs Clinical Significance**
402
- - p<0.05 does not guarantee clinical importance
403
- - Small effects can be statistically significant with large samples
404
- - Large effects can be non-significant with small samples
405
- - Consider effect size magnitude and confidence interval width
406
-
407
- **Number Needed to Treat (NNT)**
408
- - NNT = 1 / absolute risk reduction
409
- - Example: 10% vs 5% event rate → ARR = 5% → NNT = 20
410
- - Interpretation: Treat 20 patients to prevent 1 event
411
- - Useful for communicating treatment benefit
412
-
413
- **Minimal Clinically Important Difference (MCID)**
414
- - Pre-defined threshold for meaningful clinical benefit
415
- - OS: Often 2-3 months in oncology
416
- - PFS: Context-dependent, often 1.5-3 months
417
- - QoL: 10-point change on 100-point scale
418
- - Response rate: Often 10-15 percentage point difference
419
-
420
- ### Contextualization
421
-
422
- - Compare to historical controls or standard of care
423
- - Consider patient population characteristics
424
- - Account for prior treatment exposure
425
- - Evaluate toxicity trade-offs
426
- - Assess quality of life impact
427
-