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OpenOnco · DIS-FL · Organ dysfunction (CrCl 25, bili 3.5×ULN)
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OpenOnco · Treatment Plan
Treatment plan — Follicular Lymphoma
PLAN-VAR-FL-ORGAN-V1 · v1 · 2026-05-12
Patient
VAR-FL-ORGAN · Algorithm: ALGO-FL-1L
DiagnosisFollicular Lymphoma
MOH / ICD-10C82.0
ICD-O-39690/3

Clinical significance of mutations (ESCAT)

Tumor-board context — the engine does not use these tiers to rank tracks
✅ Covered biomarkers (matched in KB)
BiomarkerVariantESCATEvidenceClinical significanceDrugsSources
No clinically actionable variants matched in this profile.
⚠️ Not included in plan
BiomarkerStatus
BIO-CD20-IHCBIO definition in KB; no ESCAT BMA entry — verify with clinician

Primary current-line option

Active surveillance (watch-and-wait)
★ DEFAULT
Indication
IND-FL-1L-WATCH
Regimen
Reason
Primary current-line option selected by ALGO-FL-1L at step 3.

Other current-line alternatives (2 tracks)

Same treatment line; review when biomarker, access, contraindication, or patient-context assumptions change.
Standard plan
Indication
IND-FL-1L-BR
Regimen
Bendamustine + Rituximab (BR), 6 cycles
Drugs + NSZU
  • Rituximab (DRUG-RITUXIMAB) 375 mg/m² · day 1 of each 28-day cycle · IV ✓ NSZU covered
  • Bendamustine (DRUG-BENDAMUSTINE) 90 mg/m² · days 1 and 2 of each 28-day cycle · IV ⚠ NSZU — not for this indication
Supportive care
SUP-ANTIEMETIC-PREMED, SUP-PJP-PROPHYLAXIS
Hard contraindications
CI-HBV-NO-PROPHYLAXIS, CI-SEVERE-CYTOPENIA-BR
Reason
Current-line alternative presented for HCP consideration
Aggressive plan
Indication
IND-FL-1L-RCHOP-AGGRESSIVE
Regimen
Rituximab + CHOP (R-CHOP), 6 cycles
Drugs + NSZU
  • Rituximab (DRUG-RITUXIMAB) 375 mg/m² · IV day 1 of each 21-day cycle · IV ✓ NSZU covered
  • Cyclophosphamide (DRUG-CYCLOPHOSPHAMIDE) 750 mg/m² · IV day 1 of each 21-day cycle · IV ⚠ NSZU — not for this indication
  • Doxorubicin (DRUG-DOXORUBICIN) 50 mg/m² · IV day 1 of each 21-day cycle · IV ⚠ NSZU — not for this indication
  • Vincristine (DRUG-VINCRISTINE) 1.4 mg/m² (capped at 2 mg total) · IV day 1 of each 21-day cycle · IV ⚠ NSZU — not for this indication
  • Prednisone (DRUG-PREDNISONE) 100 mg · PO days 1-5 of each 21-day cycle · PO ⚠ NSZU — not for this indication
Supportive care
SUP-PJP-PROPHYLAXIS, SUP-TLS-PROPHYLAXIS, SUP-ANTIEMETIC-PREMED
Hard contraindications
CI-HBV-NO-PROPHYLAXIS, CI-LVEF-LOW-FOR-ANTHRACYCLINE
Reason
Current-line alternative presented for HCP consideration

Pre-treatment investigations

Investigations before treatment start · critical / standard / desired · merged across tracks
IDNamePriorityCategoryWhere to orderNeeded for
TEST-BM-ASPIRATEBone Marrow AspirateCriticalhistologyall tracks
TEST-BM-TREPHINEBone Marrow TrephineCriticalhistologyall tracks
TEST-CBCComplete Blood Count with DifferentialCriticallaball tracks
TEST-CD20-IHCCD20 ImmunohistochemistryCriticalhistologyCSD Lab ✓ (code TBC)all tracks
TEST-CMPComprehensive Metabolic PanelCriticallaball tracks
TEST-FISH-PANELFISH (Fluorescence In Situ Hybridization)CriticalgenomicCSD Lab ✓ (code TBC)aggressive, standard
TEST-FLOW-CYTOMETRYFlow CytometryCriticalhistologyCSD Lab ✓ (code TBC)all tracks
TEST-HBV-SEROLOGYHepatitis B Serology Panel (HBsAg, anti-HBc total, anti-HBs)Criticallaball tracks
TEST-HCV-ANTIBODYHCV AntibodyCriticallabaggressive, standard
TEST-HIV-SEROLOGYHIV Antibody/AntigenCriticallabaggressive, standard
TEST-LDHLactate DehydrogenaseCriticallaball tracks
TEST-LFTLiver Function Tests (ALT, AST, bilirubin, ALP, GGT, albumin)Criticallaball tracks
TEST-LN-EXCISIONAL-BIOPSYExcisional LN BiopsyCriticalhistologyall tracks
TEST-PREGNANCYBeta-HCGCriticallabaggressive, standard
TEST-B2-MICROGLOBULINBeta-2 MicroglobulinStandardlaball tracks
TEST-ECHOEchocardiographyStandardimagingaggressive
TEST-PET-CTFDG PET/CT (whole body)Standardimagingall tracks

Red flags — PRO / CONTRA aggressive

PRO-AGGRESSIVE

Triggers that push toward the aggressive track
  • Follicular lymphoma meeting GELF criteria for high tumor burden — any of: nodal mass ≥7 cm; ≥3 nodal sites each ≥3 cm; B-symptoms; splenomegaly below umbilicus; pleural/peritoneal effusion; cytopenia (Hb <10, plt <100K, ANC <1.5K) attributable to lymphoma; LDH >ULN; β2M elevated; rapidly progressive diseaseRF-FL-HIGH-TUMOR-BURDEN-GELF
  • Follicular lymphoma with clinical features concerning for transformation to aggressive lymphoma (typically DLBCL): rapid disease progression, isolated rapidly-growing nodal mass, sudden LDH rise, new B-symptoms, hypercalcemia, extranodal involvement onsetRF-FL-TRANSFORMATION-SUSPECT

CONTRA-AGGRESSIVE

Hard contraindications to escalation
  • Active or latent HBV without antiviral prophylaxis is an absolute contraindication to starting B-cell-depleting / immunomodulatory monoclonal antibody therapy (anti-CD20, anti-CD30 ADC, anti-CD38). Severe HBV reactivation hepatitis risk including fulminant hepatic failure.CI-HBV-NO-PROPHYLAXIS
  • Pre-treatment LVEF <50% is an absolute contraindication to anthracycline-containing regimens (R-CHOP, Pola-R-CHP, ABVD, BV-AVD, etc.). Cardiotoxicity from doxorubicin is dose-cumulative and often irreversible; starting with already-impaired function risks acute decompensation.CI-LVEF-LOW-FOR-ANTHRACYCLINE

What NOT to do

Explicit prohibitive rules, each grounded in a regimen / supportive care / contraindication entity
Active surveillance (watch-and-wait) (IND-FL-1L-WATCH)
  • Do not start treatment in an asymptomatic patient without GELF criteria — no RCT evidence of mortality reduction, only excess toxicity + immunosuppression.
  • Do not skip CD20 + flow + IHC confirmation of diagnosis before W&W — without an accurate diagnosis W&W is not justified.
  • Do not skip re-biopsy in a rapidly-growing dominant lesion or PET hot-spot — transformation to DLBCL requires R-CHOP.
  • Do not order routine surveillance imaging — clinical monitoring + labs; PET-CT only on indication.
Standard plan (IND-FL-1L-BR)
  • Do not start without HBV screening + entecavir prophylaxis in HBsAg+ or anti-HBc+.
  • Do not prescribe in severe baseline cytopenia (CI-SEVERE-CYTOPENIA-BR).
  • Do not use full-dose bendamustine at FIB-4 > 3.25 — reduce to 70 mg/m².
  • Do not forget PJP prophylaxis (cotrimoxazole) — continue ≥6 mo after the last dose of anti-CD20.
  • Do not delay imaging-driven response through 4 cycles — interim PET if there is concern about transformation or progression.
Aggressive plan (IND-FL-1L-RCHOP-AGGRESSIVE)
  • Do not prescribe without re-biopsy when transformation is suspected — accurate histology determines treatment.
  • Do not prescribe without baseline LVEF ≥50% — anthracycline cardiotoxicity.
  • Do not start without HBV screening + entecavir prophylaxis in HBsAg+ or anti-HBc+.
  • Do not administer vincristine intrathecally — FATAL.

Monitoring schedule

Monitoring schedule by treatment phase

Standard plan · MON-BR-REGIMEN

PhaseWindowTestsCheckpoints
baselineWithin 2 weeks before cycle 1TEST-CBC, TEST-LFT, TEST-LDH, TEST-HBV-SEROLOGY, TEST-FIB4, TEST-CD20-IHC, TEST-PET-CT
  • Confirm CD20+ histology
  • Confirm HBV status and prophylaxis plan
  • FIB-4 + LFT determine bendamustine dose adjustment
on_treatmentDay 1 of every 28-day cycleTEST-CBC, TEST-LFT
  • ANC ≥ 1500/µL and platelets ≥ 75K before each cycle (delay otherwise)
  • ALT/AST trend (rising values may signal HBV reactivation or hepatotoxicity)
response_assessmentAfter cycles 3 and 6TEST-PET-CT, TEST-LDH
  • Lugano response criteria (CR, PR, SD, PD)
  • If <PR after cycle 3 → consider regimen change
follow_up_shortEvery 3 months for 2 years post-treatmentTEST-CBC, TEST-LFT, TEST-LDH
  • Surveillance for relapse
  • HBV reactivation monitoring continues for 12 months post anti-CD20
follow_up_longEvery 6 months years 3-5TEST-CBC, TEST-LFT

Aggressive plan · MON-R-CHOP-REGIMEN

PhaseWindowTestsCheckpoints
baselineWithin 2 weeks before cycle 1TEST-CBC, TEST-CMP, TEST-LFT, TEST-LDH, TEST-B2-MICROGLOBULIN, TEST-HBV-SEROLOGY, TEST-HCV-ANTIBODY, TEST-HIV-SEROLOGY, TEST-PET-CT, TEST-LN-EXCISIONAL-BIOPSY, TEST-FLOW-CYTOMETRY, TEST-CD20-IHC, TEST-ECHO, TEST-PREGNANCY, TEST-BM-ASPIRATE, TEST-BM-TREPHINE
  • Confirm CD20+ DLBCL histology; rule out double-hit (FISH for MYC/BCL2/BCL6)
  • Confirm HBV status + entecavir prophylaxis plan if HBsAg+ or anti-HBc+
  • Baseline LVEF ≥50% before doxorubicin
  • IPI calculation documented (age, ECOG, LDH, stage, extranodal sites)
  • CNS-IPI calculation if anatomic risk sites or composite score concerning
  • Fertility preservation discussion (sperm banking / oocyte cryo) for childbearing-age
on_treatmentDay 1 of every 21-day cycleTEST-CBC, TEST-CMP, TEST-LFT
  • ANC ≥1500 + platelets ≥100K before each cycle (delay or G-CSF if not)
  • Neuropathy grade documented (CTCAE) — vincristine modification if ≥2
  • LVEF re-check after cumulative doxorubicin ~300 mg/m²
interim_response_assessmentAfter cycles 2-4 (interim PET-CT)TEST-PET-CT, TEST-LDH
  • Lugano response criteria + Deauville score
  • If Deauville 4-5 with mass progression → consider salvage or trial
end_of_treatmentAfter cycle 6 (within 6-8 weeks)TEST-PET-CT, TEST-CBC, TEST-CMP, TEST-LDH
  • Confirm CR vs PR vs SD vs PD by Lugano/Deauville
  • Begin survivorship plan: cardiac surveillance schedule, vaccination catch-up, second-cancer screening
follow_up_shortEvery 3 months × 2 years post-treatmentTEST-CBC, TEST-CMP, TEST-LFT, TEST-LDH
  • Surveillance for relapse (~40% relapse risk by 2 years overall)
  • HBV reactivation monitoring continues for 12 months post anti-CD20
follow_up_longEvery 6 months years 3-5, then annuallyTEST-CBC, TEST-LFT, TEST-ECHO
  • Late cardiomyopathy screening (LVEF) annually if cumulative dox >300
  • Annual second-malignancy screening (skin, breast, etc. age-appropriate)

Timeline

Treatment timeline — derived from regimen + monitoring schedule

Standard plan

Baseline
Within 2 weeks before cycle 1
Induction · Bendamustine + Rituximab (BR), 6 cycles
28-day cycles × 6
Response assessment
After cycles 3 and 6
Follow-up
Every 3 months for 2 years post-treatment

Aggressive plan

Baseline
Within 2 weeks before cycle 1
Induction · Rituximab + CHOP (R-CHOP), 6 cycles
21-day cycles × 6 (with consideration of 2-month interim PET-CT after cycles 2-4)
Response assessment
After cycles 2-4 (interim PET-CT)
Follow-up
Every 3 months × 2 years post-treatment

MDT brief

Discussion questions (4, 2 blocking)

  • BLOCKING OQ-CD20-CONFIRMATION
    Is CD20+ status confirmed by histology (IHC)? Without CD20+, rituximab/obinutuzumab are not indicated.
    Anti-CD20 therapy is the backbone of most lines of treatment; absence of CD20 expression fully changes the regimen.
    → pathologist
  • OQ-STAGING-COMPLETE
    Has complete staging been done (Lugano + PET/CT or CT)?
    Prognosis and track selection depend on stage and tumor burden.
    → radiologist
  • OQ-LDH-CURRENT
    What is the current LDH? Marker of tumor burden and transformation.
    LDH is part of the prognostic indices of indolent lymphomas.
    → hematologist
  • BLOCKING OQ-BIOMARKER-FL-FLIPI
    What is the status of Follicular Lymphoma International Prognostic Index (FLIPI) (BIO-FL-FLIPI)? It is required by track(s): IND-FL-1L-WATCH, IND-FL-1L-BR, IND-FL-1L-RCHOP-AGGRESSIVE. Expected value: FLIPI 0-2 (low/intermediate-risk) — watch-and-wait reserved for low-burden, asymptomatic disease (GELF-criteria-negative); high-FLIPI typically routes to active treatment.
    A treatment-track biomarker requirement is missing from the patient profile; the MDT should verify the test result, method, specimen, and date before relying on this option.
    → medical_oncologist

MDT talk tree (5 steps)

#OwnerTopicAction
1medical_oncologistBiomarker status BLOCKINGWhat is the status of Follicular Lymphoma International Prognostic Index (FLIPI) (BIO-FL-FLIPI)? It is required by track(s): IND-FL-1L-WATCH, IND-FL-1L-BR, IND-FL-1L-RCHOP-AGGRESSIVE. Expected value: FLIPI 0-2 (low/intermediate-risk) — watch-and-wait reserved for low-burden, asymptomatic disease (GELF-criteria-negative); high-FLIPI typically routes to active treatment.
2pathologistPathology confirmation BLOCKINGIs CD20+ status confirmed by histology (IHC)? Without CD20+, rituximab/obinutuzumab are not indicated.
3hematologistStaging / disease burden What is the current LDH? Marker of tumor burden and transformation.
4radiologistStaging / disease burden Has complete staging been done (Lugano + PET/CT or CT)?
5clinical_pharmacistSpecialist review Chemoimmunotherapy regimen — drug-drug interactions, dose adjustments, premedication.

Skills (required) — mandatory virtual specialists (1)

  • Hematologist / oncohematologist required
    Lymphoma diagnosis — leading specialty for treatment management.
    Owns: OQ-LDH-CURRENT

Skills (recommended) — for consideration (2)

  • Clinical pharmacist recommended
    Chemoimmunotherapy regimen — drug-drug interactions, dose adjustments, premedication.
  • Pathologist (general) recommended
    Confirm lymphoma histology + assess transformation risk (DLBCL/Richter).
    Owns: OQ-CD20-CONFIRMATION

Data quality

Incomplete for default-track review. Default-track review is incomplete until required biomarker gaps are resolved.
  • Biomarker coverage: 1/2 known (50%), 1 missing, 1 default-track gaps
  • Missing critical: cd20_ihc_status, lugano_stage
  • Missing recommended: ldh_ratio_to_uln, fib4_index, pet_ct_date
  • Unevaluated RedFlags: RF-FL-EZH2-Y641-ACTIONABLE, RF-FL-FRAILTY-AGE, RF-FL-HIGH-TUMOR-BURDEN-GELF, RF-FL-INFECTION-SCREENING, RF-FL-ORGAN-DYSFUNCTION, RF-FL-TRANSFORMATION-SUSPECT, RF-FOLLICULAR-TRANSFORMATION, RF-GELF-CRITERIA-MET, RF-GELF-LOW-BURDEN

Missing data for doctor action

PriorityClinical itemOwnerWhy it mattersNext actionBlocks
CRITICALCD20 IHC status
cd20_ihc_status
pathologistConfirms CD20-directed therapy is biologically appropriate.Verify CD20 IHC result, specimen, method, and report date.-
CRITICALLugano stage
lugano_stage
radiologistDefines lymphoma extent and supports tumor-burden and response-assessment decisions.Document Lugano stage from PET/CT or contrast CT staging.-
RECOMMENDEDLDH ratio to ULN
ldh_ratio_to_uln
medical_oncologistSupports prognostic scoring and aggressive-biology flags.Enter LDH with local upper limit of normal.-
RECOMMENDEDFIB-4 liver fibrosis index
fib4_index
infectious_disease_hepatologyScreens hepatic fibrosis risk before hepatotoxic therapy or antiviral coordination.Calculate FIB-4 from age, AST, ALT, and platelet count.-
RECOMMENDEDPET/CT date
pet_ct_date
radiologistShows whether baseline staging is recent enough for treatment planning and later response comparison.Document baseline PET/CT date or explain alternative staging modality.-
Missing biomarkerLabelMDT ownerDefault trackRequired byNext action
BIO-FL-FLIPIFollicular Lymphoma International Prognostic Index (FLIPI)medical_oncologistyesIND-FL-1L-WATCH, IND-FL-1L-BR, IND-FL-1L-RCHOP-AGGRESSIVEVerify result, method, specimen, and report date before sign-off. Expected/constraint: FLIPI 0-2 (low/intermediate-risk) — watch-and-wait reserved for low-burden, asymptomatic disease (GELF-criteria-negative); high-FLIPI typically routes to active treatment
Technical MDT skill metadata (3/16 activated in this plan)
All registered virtual specialists. ✓ — activated for this case; ○ — not activated (available for other clinical scenarios).
Specialistskill_idVersionLast reviewedSign-offsDomain
Cellular therapy specialist (CAR-T)cellular_therapy_specialistv0.1.02026-04-250cellular_therapy
Clinical pharmacistclinical_pharmacistv0.1.02026-04-250clinical_pharmacy
Hematologist / oncohematologisthematologistv0.1.02026-04-250hematology_oncology
Hematopathologist (lymphoma / leukemia / myeloma)hematopathologistv0.1.02026-04-250hematopathology
Infectious disease / hepatologyinfectious_disease_hepatologyv0.1.02026-04-250infectious_diseases
Medical oncologist (solid-tumor chemotherapist)medical_oncologistv0.1.02026-04-250solid_oncology
Molecular geneticist / molecular oncologistmolecular_geneticistv0.1.02026-04-250molecular_oncology
Palliative carepalliative_carev0.1.02026-04-250palliative_care
Pathologist (general)pathologistv0.1.02026-04-250pathology
Primary care / family physicianprimary_carev0.1.02026-04-250primary_care
Psycho-oncologistpsychologistv0.1.02026-04-250psychosocial
Radiation oncologistradiation_oncologistv0.1.02026-04-250radiation_oncology
Radiologistradiologistv0.1.02026-04-250diagnostic_imaging
Social worker / case managersocial_worker_case_managerv0.1.02026-04-250psychosocial
Surgical oncologistsurgical_oncologistv0.1.02026-04-250surgical_oncology
Transplant specialist (BMT)transplant_specialistv0.1.02026-04-250cellular_therapy

Sources cited

Experimental options (clinical trials)

Last synced: 2026-05-12 · ctgov.

No active trials matched this scenario in ctgov.

Option availability in Ukraine

Per-track UA registration · NSZU · cost · access pathway. Render-time metadata; engine selection does not depend on these fields (CHARTER §8.3).
OptionUA registrationNSZUCost orientationAccess pathway
Active surveillance (watch-and-wait)
No regimen components on this track — availability unknown
— unknown— unknown₴-? — verify pathwaynot recorded
Standard plan
Bendamustine + Rituximab (BR), 6 cycles (REG-BR-STANDARD)
✓ registered✓ covered₴-? — verify pathwayNSZU formulary
Aggressive plan
Rituximab + CHOP (R-CHOP), 6 cycles (REG-R-CHOP)
✓ registered✓ covered₴-? — verify pathwayNSZU formulary

Cost information is orientation. Verify with a specific pharmacy / foundation / trial site. Status updated: 2026-05-12.

plan_id: PLAN-VAR-FL-ORGAN-V1 | version: 1 | generated: 2026-05-12T18:41:26.397454+00:00
Per FDA non-device CDS positioning (CHARTER §15): Outpatient oncology treatment planning to support tumor-board discussion. Not a medical device; not for autonomous clinical decision-making.
Per FDA non-device CDS positioning (CHARTER §15): Both treatment options below are presented for review. The engine's selection of a 'recommended' default does not constitute a clinical decision. Final treatment selection requires HCP judgment incorporating information not available to the system.
This document is an informational resource supporting tumor-board discussion (per CHARTER §11). It is not a system that makes clinical decisions. Every recommendation must be verified by the treating physician.