managing-gynecologic-oncology

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Structures gynecologic cancer evaluation with staging, treatment planning, and surveillance. Use when managing gynecologic cancers, staging ovarian/uterine malignancies, or planning treatment.

CaseMark By CaseMark schedule Updated 4/20/2026

name: managing-gynecologic-oncology language: en description: Structures gynecologic cancer evaluation with staging, treatment planning, and surveillance. Use when managing gynecologic cancers, staging ovarian/uterine malignancies, or planning treatment. tags:

  • management
  • obstetrics-and-gynecology
  • treatment
  • valuation metadata: author: casemark practice_areas:
    • Obstetrics
    • Gynecology
    • Maternal-Fetal Medicine document_types:
    • Management Report skill_modes:
    • Management
    • Coordination

Managing Gynecologic Oncology

Structures gynecologic cancer evaluation with FIGO staging, multidisciplinary treatment planning, and surveillance protocols for endometrial, ovarian, cervical, and vulvar malignancies.

Why This Skill Exists

Gynecologic cancers — endometrial, ovarian, cervical, vulvar, and vaginal — collectively account for over 115,000 new cases and 34,000 deaths annually in the United States. Endometrial cancer is the most common gynecologic malignancy (incidence rising with the obesity epidemic), while ovarian cancer has the highest mortality due to late-stage diagnosis. FIGO staging is the international standard for all gynecologic malignancies and was updated for endometrial cancer in 2023 and cervical cancer in 2018.

Accurate staging determines treatment (surgery, chemotherapy, radiation, or combination), eligibility for clinical trials, and prognosis. Molecular classification (particularly for endometrial cancer — POLE, MSI-H, CN-low, CN-high/p53-abnormal) is now integrated into treatment planning. This skill ensures that evaluation, staging, and treatment planning follow NCCN and SGO/FIGO guidelines.


Checkpoint A: Pre-Draft Intake (Mandatory)

  1. Cancer type — endometrial, ovarian/fallopian tube/peritoneal, cervical, vulvar, vaginal, GTD? (Default: from pathology)
  2. Histologic type and grade — specific histology (endometrioid, serous, clear cell, mucinous, squamous, etc.) and differentiation grade? (Default: from pathology report)
  3. FIGO stage — current staging or pre-surgical estimated stage? (Default: from staging workup)
  4. Molecular markers — MSI/MMR status, p53 IHC, POLE mutation, ER/PR status, HER2, BRCA1/2, PD-L1? (Default: from pathology/genetic testing)
  5. Imaging — CT, MRI, PET-CT findings? (Default: from radiology reports)
  6. Tumor markers — CA-125, HE4, AFP, βhCG, inhibin (depending on tumor type)? (Default: from lab results)
  7. Performance status — ECOG performance status? (Default: from clinical assessment)
  8. Fertility preservation desire — relevant for early-stage cancers in young patients? (Default: from patient discussion)

Documents to Request

  • Pathology reports (biopsy and surgical specimens) with molecular testing
  • Operative reports (staging surgery, debulking)
  • Cross-sectional imaging (CT chest/abdomen/pelvis, MRI pelvis, PET-CT)
  • Tumor marker levels (serial if available)
  • Genetic testing results (germline BRCA, Lynch/MMR, somatic profiling)
  • Multidisciplinary tumor board recommendations
  • Prior treatment records (chemotherapy, radiation)
  • Performance status documentation

Step 1: Endometrial Cancer — FIGO 2023 Staging and Management

FIGO 2023 Staging (Surgical)

Stage Description
IA Tumor limited to endometrium or < 50% myometrial invasion
IB ≥ 50% myometrial invasion
IC Invasion of cervical stroma (formerly stage II)
II Tumor beyond uterus to ovaries, fallopian tubes, broad ligament, or vagina
IIIA Tumor invading uterine serosa or adnexa
IIIB Vaginal or parametrial involvement
IIIC1 Pelvic lymph node metastasis
IIIC2 Para-aortic lymph node metastasis
IVA Invasion of bladder or bowel mucosa
IVB Distant metastasis

Molecular Classification (The Cancer Genome Atlas — TCGA)

Subtype Prognosis Treatment Implications
POLE ultramutated Excellent (even if high-grade histology) May de-escalate adjuvant therapy
MSI-high / MMR-deficient Intermediate-favorable Checkpoint immunotherapy (pembrolizumab) if advanced; Lynch syndrome screening
Copy-number low (CN-L) Intermediate Standard stage-based adjuvant therapy
Copy-number high (CN-H) / p53-abnormal Poor Aggressive adjuvant therapy (chemo + radiation); clinical trials

Standard Surgical Staging

  • Total hysterectomy with bilateral salpingo-oophorectomy (TH/BSO)
  • Sentinel lymph node mapping (preferred) or full pelvic/para-aortic lymphadenectomy
  • Peritoneal washings
  • Omental sampling for serous, clear cell, or carcinosarcoma histology

Step 2: Ovarian Cancer — FIGO Staging and Management

FIGO Staging (Surgical)

Stage Description
I Limited to ovaries/fallopian tubes
IA One ovary, capsule intact, no surface involvement, negative washings
IB Both ovaries, capsule intact
IC Capsule rupture, surface involvement, or positive washings
II Pelvic extension
III Peritoneal metastasis beyond pelvis and/or retroperitoneal nodes
IIIC Peritoneal metastasis > 2 cm and/or retroperitoneal nodes
IV Distant metastasis (liver parenchymal, extra-abdominal)

Management Principles

  • Primary debulking surgery (PDS): Goal is R0 (no visible residual disease) — complete cytoreduction is the strongest predictor of survival
  • Neoadjuvant chemotherapy (NACT): Carboplatin + paclitaxel × 3 cycles → interval debulking surgery → 3 more cycles (for patients unlikely to achieve R0 at PDS)
  • BRCA-mutated or HRD-positive: PARP inhibitor maintenance (olaparib, niraparib) after platinum response
  • CA-125 monitoring: Serial values during and after treatment; GCIG criteria for progression (doubling from nadir and above upper limit of normal)

Step 3: Cervical Cancer — FIGO 2018 Staging and Management

FIGO 2018 Staging (Now Allows Imaging and Pathology)

Stage Description
IA1 Stromal invasion ≤ 3 mm depth
IA2 Stromal invasion > 3 mm and ≤ 5 mm depth
IB1 Clinically visible ≤ 2 cm
IB2 Clinically visible > 2 cm and ≤ 4 cm
IB3 Clinically visible > 4 cm
IIA Upper 2/3 vagina, no parametrial invasion
IIB Parametrial invasion
IIIA Lower 1/3 vagina
IIIB Pelvic sidewall / hydronephrosis
IIIC1 Pelvic lymph node metastasis
IIIC2 Para-aortic lymph node metastasis
IVA Bladder or rectal mucosal invasion
IVB Distant metastasis

Treatment by Stage

  • IA1 (no LVSI): Cone biopsy with negative margins (fertility-sparing) or simple hysterectomy
  • IA2–IB1: Radical hysterectomy + pelvic lymphadenectomy; or radical trachelectomy (fertility-sparing)
  • IB2–IIA: Radical hysterectomy vs. primary chemoradiation (equivalent outcomes)
  • IIB–IVA: Primary chemoradiation (cisplatin weekly + external beam + brachytherapy)
  • IVB: Systemic chemotherapy ± pembrolizumab (PD-L1 positive or MSI-H); bevacizumab per GOG 240

Step 4: Surveillance Protocols

Cancer Type Surveillance Schedule Key Assessments
Endometrial Q3–6 months × 2 years, then Q6–12 months × 3 years Symptom review, pelvic exam, vaginal cuff cytology (if risk factors), imaging only if symptomatic
Ovarian Q2–4 months × 2 years, then Q3–6 months × 3 years CA-125, exam, CT if rising markers or symptoms
Cervical Q3–4 months × 2 years, then Q6 months × 3 years Pap smear (if treated with surgery), pelvic exam, imaging if indicated
Vulvar Q6 months × 2 years, then annually Vulvar exam, biopsy any suspicious lesions

Checkpoint B: Post-Draft Alignment (Mandatory)

  1. Is the FIGO stage correctly assigned using the most current staging system (endometrial 2023, cervical 2018)?
  2. Is histologic type and grade documented with molecular classification for endometrial cancer?
  3. Does the treatment plan align with NCCN guidelines for the stage and histology?
  4. Are molecular markers documented — MSI, p53, BRCA, PD-L1 as applicable?
  5. Is the surveillance schedule specified with appropriate intervals and assessments?

Quality Audit

  • Cancer type and histologic subtype documented from pathology
  • FIGO stage assigned with supporting evidence (imaging, surgical findings, pathology)
  • Tumor grade (well, moderately, poorly differentiated) documented
  • Molecular markers documented (MSI/MMR, p53, POLE, BRCA, HER2, PD-L1 as applicable)
  • Imaging staging documented (CT, MRI, PET-CT findings)
  • Tumor markers documented (CA-125, HE4, others as applicable)
  • Surgical staging completeness documented (LN assessment, washings, omentum)
  • Residual disease status documented for ovarian cancer (R0, R1, R2)
  • Multidisciplinary tumor board discussion documented
  • Adjuvant therapy plan specified with regimen and cycle count
  • Genetic counseling referral documented (Lynch, BRCA, when indicated)
  • Performance status documented (ECOG)
  • Surveillance plan documented with intervals and assessments
  • Fertility preservation discussion documented (if applicable)

Guidelines

  1. Use the correct FIGO staging year — endometrial 2023, cervical 2018, ovarian 2014. Misapplying staging systems leads to incorrect treatment.
  2. Molecular classification is now standard for endometrial cancer — POLE, MSI, p53, and CN status must be obtained to guide adjuvant therapy decisions.
  3. Optimal cytoreduction is the goal in ovarian cancer — document residual disease status (R0, < 1 cm, > 1 cm) as it drives prognosis.
  4. Test all endometrial cancers for MMR/MSI — per NCCN, universal screening identifies Lynch syndrome and eligibility for immunotherapy.
  5. Do not skip genetic referral — all ovarian cancer patients should be offered germline BRCA testing; all endometrial cancer patients with MSI-H or age < 50 should be evaluated for Lynch.
  6. Document tumor board decisions — multidisciplinary review is standard of care and should be recorded with attending specialties and recommendations.
  7. Fertility-sparing options exist — for early-stage endometrial (grade 1, IA) and cervical (IA1–IB1) cancers, conservative management can be offered after thorough counseling.
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