--- name: mpn-research-assistant description: "Myeloproliferative neoplasm (MPN) research expertise including JAK2/CALR/MPL mutations, myelofibrosis, polycythemia vera, essential thrombocythemia. Use for MPN literature search, driver mutation analysis, PPM1D pathway analysis, fibrosis markers, megakaryocyte biology, clinical trial data interpretation, and translational research." license: Proprietary --- # MPN Research Assistant ## Disease Classification ### WHO 2022 Classification - **Polycythemia Vera (PV)**: JAK2V617F (95%), JAK2 exon 12 (3%) - **Essential Thrombocythemia (ET)**: JAK2V617F (55%), CALR (25%), MPL (5%) - **Primary Myelofibrosis (PMF)**: JAK2V617F (55%), CALR (25%), MPL (8%) - **Pre-PMF**: Early fibrotic stage, better prognosis - **Overt PMF**: Grade 2-3 fibrosis, splenomegaly ### Driver Mutations | Mutation | Gene Location | Mechanism | VAF Significance | |----------|--------------|-----------|------------------| | JAK2V617F | 9p24.1 | Constitutive JAK-STAT activation | >50% → poor prognosis | | CALR (type 1) | 19p13.2 | 52bp deletion, MPL activation | Better prognosis | | CALR (type 2) | 19p13.2 | 5bp insertion, MPL activation | Intermediate | | MPL W515L/K | 1p34.2 | TPO-independent signaling | Thrombocytosis | ### High Molecular Risk (HMR) Mutations - ASXL1, EZH2, SRSF2, IDH1/2, U2AF1 - ≥2 HMR mutations = very high risk ## PPM1D Pathway Analysis ### Expression Patterns - 83.9-fold overexpression vs normal donors (p=0.0002) - JAK2V617F+ > CALR+ expression (43.4x vs 13.4x, p=0.01) - Mutation frequency: 1.9% (8th most common in MPNs) ### Therapeutic Targets ```python ppm1d_targets = { 'PPM1D inhibitors': ['GSK2830371', 'SL-176'], 'MDM2 inhibitors': ['navtemadlin (KRT-232)', 'idasanutlin'], 'Combination': ['PPM1D + MDM2 (synergistic)'], } # p53 pathway restoration mechanism = """ PPM1D inhibition → ↑p53 phosphorylation → ↑p53 stabilization → ↑DNA damage response → ↑apoptosis in mutant clones """ ``` ### Clinical Trial Data (BOREAS) - Navtemadlin: 15% SVR35, 24% TSS50 - CD34+ reduction: 68-76% at 24-36 weeks - VAF reduction: 21% achieved ≥50% decrease - Fibrosis improvement: 45% by one grade ## Megakaryocyte Subtypes in MPNs ```python mk_subtypes = { 'Endomitotic MKs': { 'markers': ['ITGA2B', 'GP1BA', 'PF4', 'TUBB1'], 'function': 'Polyploidization', 'mpn_change': 'Dysregulated endomitosis' }, 'Platelet-Generating MKs': { 'markers': ['VWF', 'F2R', 'GP9', 'SELP'], 'function': 'Proplatelet formation', 'mpn_change': 'Abnormal platelet production' }, 'HSC Niche-Supporting MKs': { 'markers': ['THPO', 'IGF1', 'CXCL12', 'ANGPT1'], 'function': 'HSC maintenance', 'mpn_change': 'Disrupted niche signaling' }, 'Inflammatory MKs': { 'markers': ['S100A8', 'S100A9', 'CHI3L1', 'CXCL8'], 'function': 'Inflammation', 'mpn_change': 'Expanded in MF' } } ``` ## Fibrosis Markers ### Psaila 2020 Fibrosis Gene Signature ```python fibrosis_genes = [ 'TGFB1', 'IL12A', 'IL1B', 'RAB37', 'TIMP1', 'APIP', 'PF4V1', 'VEGFA', 'FBLN2', 'SFRP1', 'COL6A2', 'COL4A2', 'COL5A1', 'PDGFRB', 'LOXL2', 'RUNX2' ] # ECM remodeling ecm_markers = ['COL1A1', 'COL3A1', 'FN1', 'LAMA1', 'LAMB1'] # Profibrotic cytokines cytokines = ['TGFB1', 'PDGF', 'VEGFA', 'IL1B', 'IL6', 'TNF'] ``` ## Prognostic Scoring Systems ### MIPSS70+ v2.0 (Myelofibrosis) | Variable | Points | |----------|--------| | Hemoglobin <10 g/dL | 2 | | Blasts ≥2% | 1 | | Constitutional symptoms | 2 | | Absence of CALR type-1 | 2 | | HMR mutations | 2 each | | Unfavorable karyotype | 3 | ### Risk Categories - Very Low: 0-1 points (10yr OS: 92%) - Low: 2-4 points - Intermediate: 5-8 points - High: 9-11 points - Very High: ≥12 points ## Data Integration Template ```python def create_mpn_patient_matrix(clinical_df, mutations_df, cytokines_df, flow_df, degs_df): """Integrate multi-modal MPN patient data.""" # Merge clinical matrix = clinical_df.copy() # Add mutation status driver_muts = ['JAK2', 'CALR', 'MPL'] hmr_muts = ['ASXL1', 'EZH2', 'SRSF2', 'IDH1', 'IDH2'] for mut in driver_muts + hmr_muts: if mut in mutations_df.columns: matrix[f'{mut}_status'] = mutations_df[mut] # Calculate HMR count matrix['HMR_count'] = matrix[[f'{m}_status' for m in hmr_muts if f'{m}_status' in matrix.columns]].sum(axis=1) # Add cytokine data for cyto in ['TGFB1', 'IL6', 'IL8']: if cyto in cytokines_df.columns: matrix[f'{cyto}_level'] = cytokines_df[cyto] # Add flow cytometry matrix['CD34_percent'] = flow_df['CD34_positive_percent'] return matrix ``` ## Key References ```python key_papers = { 'Williams_2022': 'Blood: Phylogenetic reconstruction of MPN evolution', 'Psaila_2020': 'Nature Medicine: Single-cell profiling of MF megakaryocytes', 'Mascarenhas_2022': 'Blood Advances: Idasanutlin in PV', 'BOREAS_2024': 'Phase III navtemadlin in MF', 'Marcellino_iPSC': 'PPM1D iPSC modeling in MPNs', 'Kanagal-Shamanna': 'Mod Pathol: i(17q) in MDS/MPN' } ``` ## PubMed Search Templates ```python mpn_search_queries = { 'ppm1d_mpn': '"PPM1D"[Title/Abstract] AND ("myeloproliferative"[Title/Abstract] OR "myelofibrosis"[Title/Abstract])', 'single_cell_mpn': '"single-cell"[Title/Abstract] AND "myeloproliferative neoplasm"[Title/Abstract]', 'jak2_calr': '(JAK2V617F OR "CALR mutation") AND myeloproliferative', 'fibrosis_mk': 'megakaryocyte[Title/Abstract] AND fibrosis[Title/Abstract] AND myelofibrosis' } ``` See `references/mpn_clinical_trials.md` for ongoing trials. See `references/mpn_mutations_database.md` for complete mutation catalog.