OpenOnco · Treatment Plan

Treatment plan — Ovarian carcinoma

PLAN-VAR-OVARIAN-RELAPSED-V1 · v1 · 2026-05-13

Patient

VAR-OVARIAN-RELAPSED · Algorithm: ALGO-OVARIAN-2L

DiagnosisOvarian carcinoma

MOH / ICD-10C56

ICD-O-38441/3; C56, C57.0, C48.1

Clinical significance of mutations (ESCAT)

Tumor-board context — the engine does not use these tiers to rank tracks

✅ Covered biomarkers (matched in KB)

Biomarker	Variant	ESCAT	Evidence	Clinical significance	Drugs	Sources
BIO-HRD-STATUS	HRD-positive — BRCA1/2 mutation OR genomic instability score (GIS) above validated threshold (Myriad MyChoice ≥42 or equivalent FoundationOne CDx HRD signature); ~50% of high-grade serous ovarian carcinoma	IA	SRC-NCCN-OVARIAN-2025 SRC-ESMO-OVARIAN-2024 Evidence cited from clinical guidelines; per-source evidence levels not yet structured. See Phase-2-of-CIViC-pivot for re-cite roadmap.	HRD-positive high-grade serous ovarian carcinoma (~50% — encompassing BRCA1/2-mutated and BRCA-WT/HRD+): PARP inhibitor maintenance after platinum response is FDA-approved 1L. Olaparib monotherapy maintenance for BRCA1/2-mutated newly-diagnosed advanced ovarian after CR/PR to platinum (SOLO-1 Moore NEJM 2018 — mPFS not reached vs 13.8 mo, HR 0.30) per SRC-NCCN-OVARIAN-2025, SRC-ESMO-OVARIAN-2024. Olaparib + bevacizumab maintenance for HRD-positive (BRCA-mut OR HRD-genomic) post-1L platinum + bevacizumab (PAOLA-1 Ray-Coquard NEJM 2019 — HRD subgroup mPFS 37 vs 17 mo, HR 0.33). Niraparib monotherapy maintenance is approved for all-comers (PRIMA Gonzalez-Martin NEJM 2019), with the strongest benefit in HRD-positive subgroup.	olaparib monotherapy maintenance (1L BRCA1/2-mut per SRC-NCCN-OVARIAN-2025, SRC-ESMO-OVARIAN-2024) olaparib + bevacizumab maintenance (1L HRD-positive non-BRCA per SRC-NCCN-OVARIAN-2025) niraparib monotherapy maintenance (1L per SRC-NCCN-OVARIAN-2025, all-comers benefit, HRD-positive strongest) rucaparib monotherapy (2L maintenance / treatment per SRC-NCCN-OVARIAN-2025)	SRC-NCCN-OVARIAN-2025 SRC-ESMO-OVARIAN-2024

⚠️ Not included in plan

Biomarker	Status
BIO-FRA	BIO definition in KB; no ESCAT BMA entry — verify with clinician

Primary current-line option

Standard plan

★ DEFAULT

Indication

IND-OVARIAN-2L-PLAT-RES-WEEKLY-PAC-BEV

Regimen

Weekly Paclitaxel + Bevacizumab (platinum-resistant recurrent ovarian, AURELIA)

Drugs + NSZU

Paclitaxel (DRUG-PACLITAXEL) 80 mg/m² · IV days 1, 8, 15, 22 of 28-day cycle · IV ✓ NSZU covered
Bevacizumab (DRUG-BEVACIZUMAB) 10 mg/kg · IV every 14 days (or 15 mg/kg every 21 days) · IV ✓ NSZU covered

Reason

Primary current-line option selected by ALGO-OVARIAN-2L at step 6.

Other current-line alternatives (8 tracks)

Same treatment line; review when biomarker, access, contraindication, or patient-context assumptions change.

Standard plan

Indication

IND-OVARIAN-2L-PLAT-SENS-CARBO-PLD-BEV

Regimen

Carboplatin + PLD + Bevacizumab (platinum-sensitive recurrent ovarian)

Drugs + NSZU

Carboplatin (DRUG-CARBOPLATIN) AUC 5 · IV day 1 every 28 days · IV ✓ NSZU covered
Pegylated liposomal doxorubicin (DRUG-PEGYLATED-LIPOSOMAL-DOXORUBICIN) 30 mg/m² · IV day 1 every 28 days · IV ⚠ Out-of-pocket
Bevacizumab (DRUG-BEVACIZUMAB) 10 mg/kg · IV every 14 days during induction; continue 15 mg/kg q21d as maintenance until progression · IV ✓ NSZU covered

Reason

Current-line alternative presented for HCP consideration

Standard plan

Indication

IND-OVARIAN-2L-PLAT-SENS-CARBO-GEM-BEV

Regimen

Carboplatin + Gemcitabine + Bevacizumab (platinum-sensitive recurrent ovarian, OCEANS regimen)

Drugs + NSZU

Carboplatin (DRUG-CARBOPLATIN) AUC 4 · IV day 1 every 21 days · IV ✓ NSZU covered
Gemcitabine (DRUG-GEMCITABINE) 1000 mg/m² · IV days 1 and 8 every 21 days · IV ✓ NSZU covered
Bevacizumab (DRUG-BEVACIZUMAB) 15 mg/kg · IV day 1 every 21 days during induction; continue as maintenance until progression · IV ✓ NSZU covered

Reason

Current-line alternative presented for HCP consideration

Aggressive plan

Indication

IND-OVARIAN-MAINT-PARPI-BRCAM-OLAPARIB

Regimen

Olaparib maintenance (HRD+ ovarian post-platinum response)

Drugs + NSZU

Olaparib (DRUG-OLAPARIB) 300 mg PO BID continuous · Continuous · PO ✓ NSZU covered

Reason

Current-line alternative presented for HCP consideration

Aggressive plan

Indication

IND-OVARIAN-MAINT-PARPI-HRD-NIRAPARIB

Regimen

Niraparib maintenance (HRD+ recurrent platinum-sensitive ovarian, NOVA / PRIMA)

Drugs + NSZU

Niraparib (DRUG-NIRAPARIB) 200 mg PO daily if baseline weight <77 kg OR platelets <150 × 10⁹/L; otherwise 300 mg PO daily (individualized starting dose per Berek et al. 2018 update) · Continuous · PO ✓ NSZU covered

Reason

Current-line alternative presented for HCP consideration

Aggressive plan

Indication

IND-OVARIAN-MAINT-PARPI-RUCAPARIB

Regimen

Rucaparib maintenance (recurrent platinum-sensitive ovarian, ARIEL3)

Drugs + NSZU

Rucaparib (DRUG-RUCAPARIB) 600 mg PO BID continuous · Continuous until progression or unacceptable toxicity · PO ✗ Not registered in UA

Reason

Current-line alternative presented for HCP consideration

Aggressive plan

Indication

IND-OVARIAN-2L-PLAT-RES-MIRVETUXIMAB

Regimen

Mirvetuximab soravtansine (FRα-high platinum-resistant ovarian, MIRASOL)

Drugs + NSZU

Mirvetuximab soravtansine (DRUG-MIRVETUXIMAB-SORAVTANSINE) 6 mg/kg AIBW (adjusted ideal body weight) · IV every 21 days until progression or unacceptable toxicity · IV ✗ Not registered in UA

Reason

Current-line alternative presented for HCP consideration

Standard plan

Indication

IND-OVARIAN-2L-PLAT-RES-PLD-BEV

Regimen

PLD + Bevacizumab (platinum-resistant recurrent ovarian, AURELIA)

Drugs + NSZU

Pegylated liposomal doxorubicin (DRUG-PEGYLATED-LIPOSOMAL-DOXORUBICIN) 40 mg/m² · IV every 28 days · IV ⚠ Out-of-pocket
Bevacizumab (DRUG-BEVACIZUMAB) 10 mg/kg · IV every 14 days (or 15 mg/kg every 21 days) · IV ✓ NSZU covered

Reason

Current-line alternative presented for HCP consideration

Palliative plan

Indication

IND-OVARIAN-2L-PLAT-RES-TOPOTECAN

Regimen

Topotecan single-agent (platinum-resistant recurrent ovarian)

Drugs + NSZU

Topotecan (DRUG-TOPOTECAN) 4 mg/m² (weekly schedule, preferred); alternative 1.5 mg/m² IV daily × 5 days q21d (5-day schedule, more myelotoxic) · IV days 1, 8, 15 of 28-day cycle (weekly), OR daily × 5 q21d (5-day) · IV ✓ NSZU covered

Reason

Current-line alternative presented for HCP consideration

Pre-treatment investigations

Investigations before treatment start · critical / standard / desired · merged across tracks

ID	Name	Priority	Category	Where to order	Needed for
TEST-CBC	Complete Blood Count with Differential	Critical	lab	—	aggressive, palliative
TEST-GERMLINE-BRCA-PANEL	Germline BRCA1/2 + HRR panel sequencing	Standard	—	CSD Lab: M089	desired (aggressive)

Red flags — PRO / CONTRA aggressive

PRO-AGGRESSIVE

Triggers that push toward the aggressive track

Folate receptor alpha (FRα) high expression (≥75% of viable tumor cells with ≥2+ membrane staining by VENTANA FOLR1 RxDx) in platinum-resistant high-grade serous ovarian carcinoma. Mirvetuximab soravtansine (MIRASOL — mPFS 5.6 vs 4.0 mo, OS 16.5 vs 12.7 mo vs investigator-choice chemo) is FDA-approved 2L+ ADC. RF-OVARIAN-FRA-HIGH-ACTIONABLE
Frailty profile precluding standard carbo+pacli + bev intensified induction in ovarian: ECOG ≥3, OR (age ≥75 + Charlson ≥3), OR composite (age ≥70 + ascites large-volume + albumin <3.0). Triggers carbo-mono OR weekly-dose-dense-pacli (less neuropathy / bone marrow). RF-OVARIAN-FRAILTY-AGE
High perioperative VTE risk in ovarian cancer: ascites + bulky pelvic mass + immobilization + ovarian cancer's intrinsic prothrombotic state (~20% VTE incidence post-cytoreduction without prophylaxis). Mandates extended LMWH prophylaxis × 28 days post-op + careful timing of bevacizumab initiation (≥28 days post-op for surgical wound healing). RF-OVARIAN-PERIOPERATIVE-VTE

CONTRA-AGGRESSIVE

Hard contraindications to escalation

What NOT to do

Explicit prohibitive rules, each grounded in a regimen / supportive care / contraindication entity

Standard plan (IND-OVARIAN-2L-PLAT-RES-WEEKLY-PAC-BEV)

Do NOT use if Grade ≥2 residual peripheral neuropathy from prior taxane — switch to PLD arm or topotecan
Do NOT add bev if patient had Grade 3-4 bev event prior, untreated CNS mets, or major surgery within 28 days
Do NOT use platinum reinduction here — PFI ≤6 mo defines platinum-resistance
Do NOT skip paclitaxel premedication (dex + diphenhydramine + ranitidine) on first cycle

Standard plan (IND-OVARIAN-2L-PLAT-SENS-CARBO-PLD-BEV)

Do NOT use this regimen if PFI ≤6 months (platinum-resistant — switch to AURELIA backbone)
Do NOT add bevacizumab if patient had a Grade 3-4 bev event in prior line, untreated CNS mets, or major surgery within 28 days
Do NOT exceed cumulative anthracycline 550 mg/m² lifetime — track exposure across all anthracycline-containing lines
Do NOT skip maintenance PARPi if BRCA1/2-mutant or HRD-positive after CR/PR — major OS-affecting omission

Standard plan (IND-OVARIAN-2L-PLAT-SENS-CARBO-GEM-BEV)

Do NOT use this regimen if PFI ≤6 months (platinum-resistant — switch to AURELIA backbone)
Do NOT skip day-8 gemcitabine reflexively for borderline cytopenias — protocol-defined reductions / G-CSF preferred over discontinuation
Do NOT add bev if patient had Grade 3-4 bev event prior, untreated CNS mets, or major surgery within 28 days
Do NOT skip maintenance PARPi if BRCA1/2-mutant or HRD-positive after CR/PR

Aggressive plan (IND-OVARIAN-MAINT-PARPI-BRCAM-OLAPARIB)

Do NOT start without confirmed CR or PR to platinum reinduction
Do NOT start without documented BRCA1/2 pathogenic / likely-pathogenic variant (germline or somatic)
Do NOT continue olaparib through Grade 3 anemia without dose reduction (300 → 250 → 200 mg BID)
Do NOT skip pre-treatment counseling on long-term MDS/AML risk (~1-2% cumulative)

Aggressive plan (IND-OVARIAN-MAINT-PARPI-HRD-NIRAPARIB)

Do NOT start without confirmed CR or PR to platinum reinduction
Do NOT use 300 mg fixed starting dose if baseline weight <77 kg OR platelets <150 — start at 200 mg (Berek 2018 individualized rule)
Do NOT continue through Grade 3-4 thrombocytopenia without dose reduction (300 → 200 → 100 mg)
Do NOT skip pre-treatment counseling on MDS/AML risk
Do NOT skip CBC monitoring weekly for first month

Aggressive plan (IND-OVARIAN-MAINT-PARPI-RUCAPARIB)

Do NOT start without confirmed CR or PR to platinum reinduction
Do NOT mistake the rucaparib transporter-mediated creatinine elevation for true nephrotoxicity (non-progressive, not a reason to stop)
Do NOT continue through Grade 3 ALT/AST elevation with bilirubin >2× ULN — hold and dose-reduce
Do NOT skip pre-treatment counseling on MDS/AML risk (PARPi class effect)

Aggressive plan (IND-OVARIAN-2L-PLAT-RES-MIRVETUXIMAB)

Do NOT start without documented FRα-high (≥75% TPS at ≥2+) by VENTANA FOLR1 RxDx assay specifically — other FRα IHC assays not validated
Do NOT start without baseline ophthalmology evaluation (slit-lamp + visual acuity)
Do NOT skip prophylactic corticosteroid + lubricant eye drops — keratopathy is the dose-limiting AE
Do NOT continue contact lens use during therapy
Do NOT start in patients with active corneal disorder or pre-existing severe keratopathy

Standard plan (IND-OVARIAN-2L-PLAT-RES-PLD-BEV)

Do NOT use this regimen if cumulative anthracycline approaches 550 mg/m² lifetime
Do NOT add bev if patient had Grade 3-4 bev event prior, untreated CNS mets, or major surgery within 28 days
Do NOT continue PLD through Grade 3 PPE without dose hold + reduction (40 → 30 mg/m²)
Do NOT use platinum reinduction here — PFI ≤6 mo defines platinum-resistance

Palliative plan (IND-OVARIAN-2L-PLAT-RES-TOPOTECAN)

Do NOT use as first platinum-resistant choice if bevacizumab is available — AURELIA backbones outperform single-agent
Do NOT use 5-day q21d schedule unless weekly is contraindicated — myelotoxicity markedly higher with no efficacy advantage
Do NOT give if CrCl <20 (renal clearance, dose-modify CrCl 20-39)
Do NOT continue if no response after 2-3 cycles — palliative track, change quickly

Timeline

Treatment timeline — derived from regimen + monitoring schedule

Standard plan

Induction · Weekly Paclitaxel + Bevacizumab (platinum-resistant recurrent ovarian, AURELIA)

28-day cycles × Until progression or unacceptable toxicity

Standard plan

Induction · Carboplatin + PLD + Bevacizumab (platinum-sensitive recurrent ovarian)

28-day cycles × 6 induction cycles, then bevacizumab maintenance until progression / unacceptable toxicity

Standard plan

Induction · Carboplatin + Gemcitabine + Bevacizumab (platinum-sensitive recurrent ovarian, OCEANS regimen)

21-day cycles × 6-10 induction cycles (per OCEANS), then bevacizumab maintenance until progression / unacceptable toxicity

Aggressive plan

Induction · Mirvetuximab soravtansine (FRα-high platinum-resistant ovarian, MIRASOL)

21-day cycles × Until progression / unacceptable toxicity

Standard plan

Induction · PLD + Bevacizumab (platinum-resistant recurrent ovarian, AURELIA)

28-day cycles × Until progression or unacceptable toxicity

Palliative plan

Induction · Topotecan single-agent (platinum-resistant recurrent ovarian)

28-day cycles × Until progression or unacceptable toxicity

MDT brief

Discussion questions (2, 0 blocking)

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
OQ-BIOMARKER-BRCA1-BRCA2-GERMLINE
What is the status of BRCA1/BRCA2 germline pathogenic variant (BIO-BRCA1-BRCA2-GERMLINE)? It is required by track(s): IND-OVARIAN-MAINT-PARPI-BRCAM-OLAPARIB. Expected value: pathogenic OR likely pathogenic (germline OR somatic).
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.
→ molecular_geneticist

MDT talk tree (4 steps)

#	Owner	Topic	Action
1	hematologist	Staging / disease burden	What is the current LDH? Marker of tumor burden and transformation.
2	molecular_geneticist	Biomarker status	What is the status of BRCA1/BRCA2 germline pathogenic variant (BIO-BRCA1-BRCA2-GERMLINE)? It is required by track(s): IND-OVARIAN-MAINT-PARPI-BRCAM-OLAPARIB. Expected value: pathogenic OR likely pathogenic (germline OR somatic).
3	clinical_pharmacist	Specialist review	Chemoimmunotherapy regimen — drug-drug interactions, dose adjustments, premedication.
4	social_worker_case_manager	Specialist review	Plan includes drugs without NSZU reimbursement — patient access pathway must be assessed.

Skills (recommended) — for consideration (3)

Clinical pharmacist recommended
Chemoimmunotherapy regimen — drug-drug interactions, dose adjustments, premedication.
Molecular geneticist / molecular oncologist recommended
Indication references an actionable genomic biomarker — mutation / target / actionability interpretation needed.
Owns: OQ-BIOMARKER-BRCA1-BRCA2-GERMLINE
Social worker / case manager recommended
Plan includes drugs without NSZU reimbursement — patient access pathway must be assessed.

Data quality

Usable with caveats. No critical default-track gap was found, but the MDT should review the listed caveats before final sign-off.

Biomarker coverage: 2/3 known (67%), 1 missing, 0 default-track gaps
Unevaluated RedFlags: RF-BREAST-OVARIAN-HRD-ASSAY-DISTINCTION, RF-OVARIAN-BRCA-MUT-ACTIONABLE, RF-OVARIAN-FRA-HIGH-ACTIONABLE, RF-OVARIAN-FRAILTY-AGE, RF-OVARIAN-HRD-ACTIONABILITY, RF-OVARIAN-HRD-POSITIVE-ACTIONABLE, RF-OVARIAN-INFECTION-SCREENING, RF-OVARIAN-PERIOPERATIVE-VTE, RF-OVARIAN-PLATINUM-RESISTANT, RF-OVARIAN-PLATINUM-SENSITIVE, RF-OVARIAN-SUBOPTIMAL-DEBULKING, RF-OVARIAN-TRANSFORMATION-PROGRESSION, RF-PAN-BRCA-SOMATIC-PARPI-CANDIDATE

Missing biomarker	Label	MDT owner	Default track	Required by	Next action
`BIO-BRCA1-BRCA2-GERMLINE`	BRCA1/BRCA2 germline pathogenic variant	molecular_geneticist	no	IND-OVARIAN-MAINT-PARPI-BRCAM-OLAPARIB	Verify result, method, specimen, and report date before sign-off. Expected/constraint: pathogenic OR likely pathogenic (germline OR somatic)

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).

Specialist	skill_id	Version	Last reviewed	Domain
Cellular therapy specialist (CAR-T)	`cellular_therapy_specialist`	v0.1.0	2026-04-25	cellular_therapy
Clinical pharmacist	`clinical_pharmacist`	v0.1.0	2026-04-25	clinical_pharmacy
Hematologist / oncohematologist	`hematologist`	v0.1.0	2026-04-25	hematology_oncology
Hematopathologist (lymphoma / leukemia / myeloma)	`hematopathologist`	v0.1.0	2026-04-25	hematopathology
Infectious disease / hepatology	`infectious_disease_hepatology`	v0.1.0	2026-04-25	infectious_diseases
Medical oncologist (solid-tumor chemotherapist)	`medical_oncologist`	v0.1.0	2026-04-25	solid_oncology
Molecular geneticist / molecular oncologist	`molecular_geneticist`	v0.1.0	2026-04-25	molecular_oncology
Palliative care	`palliative_care`	v0.1.0	2026-04-25	palliative_care
Pathologist (general)	`pathologist`	v0.1.0	2026-04-25	pathology
Primary care / family physician	`primary_care`	v0.1.0	2026-04-25	primary_care
Psycho-oncologist	`psychologist`	v0.1.0	2026-04-25	psychosocial
Radiation oncologist	`radiation_oncologist`	v0.1.0	2026-04-25	radiation_oncology
Radiologist	`radiologist`	v0.1.0	2026-04-25	diagnostic_imaging
Social worker / case manager	`social_worker_case_manager`	v0.1.0	2026-04-25	psychosocial
Surgical oncologist	`surgical_oncologist`	v0.1.0	2026-04-25	surgical_oncology
Transplant specialist (BMT)	`transplant_specialist`	v0.1.0	2026-04-25	cellular_therapy

Sources cited

SRC-ARIEL3-COLEMAN-2017: Rucaparib maintenance treatment for recurrent ovarian carcinoma after response to platinum therapy (ARIEL3): a randomised, double-blind, placebo-controlled, phase 3 trial (2017)
SRC-AURELIA-PUJADE-LAURAINE-2014: Bevacizumab combined with chemotherapy for platinum-resistant recurrent ovarian cancer: The AURELIA open-label randomized phase III trial (2014)
SRC-ESMO-OVARIAN-2024: ESMO Ovarian Cancer Clinical Practice Guideline (2024)
SRC-GOG0213-COLEMAN-2017: Bevacizumab and paclitaxel-carboplatin chemotherapy and secondary cytoreduction in recurrent, platinum-sensitive ovarian cancer (NRG Oncology/Gynecologic Oncology Group study GOG-0213): a multicentre, open-label, randomised, phase 3 trial (2017)
SRC-MIRASOL-MOORE-2024: Mirvetuximab Soravtansine in FRα-Positive, Platinum-Resistant Ovarian Cancer (2024)
SRC-NCCN-OVARIAN-2025: NCCN Ovarian Cancer (v.2.2025)
SRC-NOVA-MIRZA-2016: Niraparib Maintenance Therapy in Platinum-Sensitive, Recurrent Ovarian Cancer (2016)
SRC-OCEANS-AGHAJANIAN-2012: OCEANS: a randomized, double-blind, placebo-controlled phase III trial of chemotherapy with or without bevacizumab in patients with platinum-sensitive recurrent epithelial ovarian, primary peritoneal, or fallopian tube cancer (2012)
SRC-PRIMA-GONZALEZ-MARTIN-2019: Niraparib in Patients with Newly Diagnosed Advanced Ovarian Cancer (2019)
SRC-SOLO2-PUJADE-LAURAINE-2017: Olaparib tablets as maintenance therapy in patients with platinum-sensitive, relapsed ovarian cancer and a BRCA1/2 mutation (SOLO2/ENGOT-Ov21): a double-blind, randomised, placebo-controlled, phase 3 trial (2017)

Experimental options (clinical trials)

Third plan track — open-enrollment trials from ClinicalTrials.gov. Render-time metadata; engine selection is not affected by this block (CHARTER §8.3). Last synced: 2026-05-13.

NCT	Title	Phase	Status	Sponsor	UA	Signals
NCT06152731	HRD Tests for Ovarian cancER	PHASE2	RECRUITING	Centre Francois Baclesse	—	Biomarker: unclear Single country
NCT06377267	Status of HRD That Lead to a Benefit From Olaparib in Combination With Bevacizumab (STROBE Trial)	PHASE2	RECRUITING	Vall d'Hebron Institute of Oncology	—	Single country
NCT06836219	Measure of Outcomes in Patients With Advanced Ovarian Cancer According to Homologous Recombination Status and Matched Therapies in a Real-world Scenario	N/A	RECRUITING	Consorzio Oncotech	—	Biomarker: unclear Single country

Verify recruitment status directly with the trial site. ctgov data can lag behind current UA-site status.

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).

Option	UA registration	NSZU	Cost orientation	Access pathway
Standard plan Weekly Paclitaxel + Bevacizumab (platinum-resistant recurrent ovarian, AURELIA) (REG-WEEKLY-PAC-BEV-OVARIAN)	✓ registered	✓ covered	₴-? — verify pathway	NSZU formulary
Standard plan Carboplatin + PLD + Bevacizumab (platinum-sensitive recurrent ovarian) (REG-CARBO-PLD-BEV-OVARIAN) 1/3 component drug(s) not on NSZU formulary	✓ registered	✗ out-of-pocket	₴-? — verify pathway	not recorded
Standard plan Carboplatin + Gemcitabine + Bevacizumab (platinum-sensitive recurrent ovarian, OCEANS regimen) (REG-CARBO-GEM-BEV-OVARIAN)	✓ registered	✓ covered	₴-? — verify pathway	NSZU formulary
Aggressive plan Olaparib maintenance (HRD+ ovarian post-platinum response) (REG-OLAPARIB-MAINT-OVARIAN)	✓ registered	✓ covered	₴-? — verify pathway	NSZU formulary
Aggressive plan Niraparib maintenance (HRD+ recurrent platinum-sensitive ovarian, NOVA / PRIMA) (REG-NIRAPARIB-MAINT-OVARIAN)	✓ registered	✓ covered	₴-? — verify pathway	NSZU formulary
Aggressive plan Rucaparib maintenance (recurrent platinum-sensitive ovarian, ARIEL3) (REG-RUCAPARIB-MAINT-OVARIAN) 1/1 component drug(s) not registered in Ukraine +1	✗ not registered	✗ out-of-pocket	₴-? — verify pathway	not recorded
Aggressive plan Mirvetuximab soravtansine (FRα-high platinum-resistant ovarian, MIRASOL) (REG-MIRVETUXIMAB-OVARIAN) 1/1 component drug(s) not registered in Ukraine +1	✗ not registered	✗ out-of-pocket	₴-? — verify pathway	not recorded
Standard plan PLD + Bevacizumab (platinum-resistant recurrent ovarian, AURELIA) (REG-PLD-BEV-OVARIAN) 1/2 component drug(s) not on NSZU formulary	✓ registered	✗ out-of-pocket	₴-? — verify pathway	not recorded
Palliative plan Topotecan single-agent (platinum-resistant recurrent ovarian) (REG-TOPOTECAN-OVARIAN)	✓ registered	✓ covered	₴-? — verify pathway	NSZU formulary
Trial · NCT06152731 HRD Tests for Ovarian cancER No UA site listed — international referral required	— unknown	— unknown	self-pay: ₴0/course	Trial sponsor
Trial · NCT06377267 Status of HRD That Lead to a Benefit From Olaparib in Combination With Bevacizumab (STROBE Trial) No UA site listed — international referral required	— unknown	— unknown	self-pay: ₴0/course	Trial sponsor
Trial · NCT06836219 Measure of Outcomes in Patients With Advanced Ovarian Cancer According to Homologous Recombination Status and Matched Therapies in a Real-world Scenario No UA site listed — international referral required	— unknown	— unknown	self-pay: ₴0/course	Trial sponsor

Cost information is orientation. Verify with a specific pharmacy / foundation / trial site. Status updated: 2026-05-13.

plan_id: PLAN-VAR-OVARIAN-RELAPSED-V1 | version: 1 | generated: 2026-05-13T10:01:52.426350+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.