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Gynecologic Pathology: Making Sense of It… (Or… What [the he*%] Do I Do With This ??) UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Lichen Sclerosis • thin, white or red epithelium – fissures, scar, fusion • • • • • possible autoimmune phenomenon “continuum”: can see with hyperplasia classic histology associated with SCC, but not “premalignant” Rx: clobetasol (0.05%): best results UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology VIN • subtypes – warty: looks like HPV – basaloid: looks like CIN – well-differentiated: formerly squamous hyperplasia • different mechanisms, epidemiology, Rx, risk – VIN (basaloid): invasive cancer: 7% (15 yr f/u) • Rx: – “squamous hyperplasia”: topical steroids – VIN: excise (laser ??), follow-up possibly imiquimod UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Paget’s Disease • atypical intraepithelial gland-type cells • raised red/pink plaque (eczema-like) • associated adenocarcinoma: – non-contiguous: 10%-26% – contiguous: 4% • Rx: excise – difficult to achieve negative margins – 2-3 cm gross margin • recurrence: 43% with WLE – 31% with vulvectomy UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Microinvasive SCC of Cervix • Stage Ia1 – < 3 mm invasion; < 7 mm lateral spread • lymph-vascular involvement does not change stage – < 3mm: not predictive of node involvement or recurrence – possibly increased recurrence if 3-5 mm depth • node involvement: – < 3 mm: ~ 1% – 3-5 mm: 2-6% • Dx: LEEP or CKC UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Margin Status • CIN • Ia1 • What to do ??? UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Margins • positive LEEP (CIN): – increased risk of recurrence (~14% - 69%) – negative margin: 5% – 25% – main risk: persistent/recurrent dysplasia • positive CKC (HGSIL): – persistence/recurrence: 22%; dysplasia * others: 5% - 16% – cancer: 1.3% (earliest: 3 years) others: 0.9% - 1.6% with prolonged follow-up if hysterectomy: 0.5% coincidental microinvasion # • Sum: positive margin – low risk of cancer (takes years) UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology * Reich D, et al. Obstet Gynecol 2002; 99: 193-196 # Burghardt E, et al. Obstet Gynecol 1980; 55: 539-545 Margins - Microinvasion • positive margin: 22% risk of residual invasion (50/51 with CIN at margin) – negative margin: 3% • If residual invasion after + margin: – Ia1: 73% – Ia2: 9% – Ib: 18% • other reports of residual invasion: 3% - 21% – definitions vary • sum: if invasion and + margin: risk of residual cancer is substantial UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Roman LD, et al. Obstet Gynecol 1997; 90: 759-764 UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Adenocarcinoma • Treated “one step higher” – Difficult to discern “early” invasion from AIS – Difficult to “measure” depth of invasion Compared to squamous – “skip” lesions • Villoglandular type – Younger patients; excellent prognosis – Usually superficially invasive – Cone biopsy may be sufficient for treatment UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Microinvasive Adenocarcinoma • Difficult to measure extent of invasion • More “accepted” outside US • Criteria: – ≤ 5 mm invasion Tumor thickness, not really depth – Obliteration of endocervical crypts – Extension beyond normal glandular area – Stromal response UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Microinvasive Adenocarcinoma Review • • • • 436 patients; 2% node metastases 15 recurrences in 436 patients 21 with cone biopsy; no recurrences Summary: CKC acceptable if ≤ 5 mm invasion, - LVS, - margins • LEEP: not acceptable Östör AG. Int J Gynecol Pathol 2000; 19: 29-38 UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Microinvasive Adenocarcinoma Conservative Treatment • Additional series – Bisseling, et al. (2007): CKC in 18 women 2 patients with Stage 1A2 No recurrences with mean F/U of 72 months – Lee, et al. (2009): CKC in 22 patients Secondary procedures in 52% (repeat CKC) Microinvasive carcinoma in 2 • Summary: CKC with careful F/U “effective” – Overall small N ….. UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Bisseling KC, et al. Gynecol Oncol 2007; 107: 424-430 Lee SW, et al. Acta Obstet Gynecol Scand 2009; 88: 209-215 UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Chronic Endometritis • key to Dx: plasma cells • 3 - 10% of AUB • historical associations: – abortion: 41% – salpingitis: 25% – IUD: 14% – fibroids: 12% – hyperplasia/cancer: 1-2% UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Chronic Endometritis Overall (%) Salpingitis 2 Postmenopausal (%) 0 IUD 4 5 Polyps 40 55 Fibroids 28 8 Hyperplasia 9 18 Carcinoma 3 8 UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Karney MY, Zahn CM. ACOG-AFD; 1997 (GAVE UP TRYING TO GET THE DAMN THING PUBLISHED !!) Endometrial Stromal Breakdown “ESB” • “estrogen withdrawal/breakthrough” • “progesterone withdrawal/breakthrough” • endometrial stromal breakdown – estrogen-stimulated, no progestin stabilization – common oligo-ovulatory pattern – focal shedding, AUB UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology ESB • pathology: – fragmented proliferative glands – fragmented proliferative stroma key distinction form menstrual pattern – “stromal balls” • Rx: – OCPs – progestin UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Iatrogenic • continuous HRT, OCP, injectables – progestin-dominant – simple glands – decidualized stroma, later atrophy • Rx: usually need estrogen – biopsy can help – don’t reflexly change “chasing your tail” UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Metaplasia • tubal – “ciliated cell change” – very common; normal and neoplastic • squamous – more common in hyperplasia • eosinophilic – “syncytial metaplasia”, “papillary surface metaplasia” – surface cells with pink cytoplasm – common in ESB – no prognostic significance UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Disordered Proliferative Endometrium • should be: – focally dilated, crowded glands – “focal” simple hyperplasia • should not be: – fragmented, breaking down • often inappropriately used for ESB UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Hyperplasia • historically: numerous terms – “cystic”, “Swiss cheese”, “adenomatous” – later: AIS, EIN • difficult to compare studies – lack of uniformity • International Society of Gynecologic Pathology and WHO (1994) – atypical vs non-atypical UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Hyperplasia - Behavior • classic study • 170 patients • followed at least 1 year before hysterectomy • mean follow-up: 13.4 years UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Kurman RJ, et al. Cancer 1985; 56: 403-412 Hyperplasia Architecture • simple – increased gland/stroma – larger glands • complex – back-to-back glands UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Nuclei (Atypia) • loss of polarity • increased N/C ratio • coarse chromatin – clumping • prominent nucleoli Behavior - Progression N regressed (%) progressed to cancer (%) 80 1 simple w/o 93 complex w/o 29 80 3 simple w/ 13 69 8 complex w/ 35 57 29 UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Kurman RJ, et al. Cancer 1985; 56: 403-412 Behavior - Progression non-atypical N progressed to cancer (%) 122 2 p = .001 atypical 48 23 •duration: •non-atypical: 10 years UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology •atypical: 4 years Hyperplasia vs Cancer Coincidental • hysterectomy soon after Dx – not followed as in “progression” studies • criteria developed to determine “invasion” • incidence of cancer at time of hysterectomy for hyperplasia: 17% – 25% UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Hyperplasia vs Cancer Criteria • cribiforming • desmoplasia (stromal response) • extensive papillary proliferation – squamous also considered • greater than ½ LPF (2.1 mm) UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Kurman RJ, Norris HJ. Cancer 1982; 49: 2547-2559 Hyperplasia vs Cancer carcinoma Grade 1 Grade 2 Grade 3 myometrial invasion inner 1/3 mid/outer 1/3 hyperplasia (%) N=89 17 100 0 0 47 * 100 0 cancer (%) N=151 50 66 24 10 72 67 33 * : all < 4 mm UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Kurman RJ, Norris HJ. Cancer 1982; 49: 2547-2559 Hyperplasia vs Cancer Coincidental Study Year N Cancer (%) Gusberg, Kaplan 1963 90 21 Tavassoli, Kraus 1978 98 25 Kurman, Norris 1982 89 17 King, et al 1984 119 15 Janicek, Rosenshein 1994 44 43 UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Hyperplasia vs Cancer Reproducibility kappa proliferative .86 hyperplasia .60 AH .47 WDC .83 overall .69 UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology • N = 100 • intraobserver agreement: .67-.85 • main atypical feature: nucleoli Kendall BS, et al. Am J Surg Pathol 1998; 22: 1012-1019 Hyperplasia vs Cancer Reproducibility % agreement cyclic 67 hyperplasia 46 AH 25 WDC 49 overall 64 UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology • N = 56 • kappa statistic: – range: .39 - .64 – mean: .52 • individual kappa statistic not reported Bergeron C, et al. Am J Surg Pathol 1999; 23: 1102-1108 Hyperplasia vs Cancer • 1975 vs 1994 WHO classification – N = 128 • overall κ (all classifications): 0.20 – 0.30 • classification reduced to 2 categories: – atypcial vs all others – κ : 0.42 – 0.59 UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Skov BG, et al. Int J Gynecol Pathol 1997; 16: 33-37 Hyperplasia vs Cancer • GOG # 167: – study of diagnosis (Phase I) – study of progestin Rx (Phase II) • problems with interpretation – wide range of diagnoses – lack of reproducibility approximately 33% agreement with community pathologic interpretation UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Hyperplasia vs Cancer Reproducibility kappa normal 0.48 hyperplasia 0.38 AH 0.28 carcinoma 0.51 overall 0.40 UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology • GOG 167 study • N = 302 • Reproducibility for study panel pathologists – experts Zaino RJ, et al. Cancer 2006; 106: 804-811 Hyperplasia vs Cancer • Study panel review of 289 “AH” specimens • Only 39.8% remained with “AH” diagnosis – 25.6% down-graded – 29.1% up-graded to carcinoma • Rate of concurrent carcinoma: 42.6% – Myometrial invasion: 30.9% – Outer half invasion: 10.6% • No consensus in 5.5% – Endometrial cancer in 62.5% of these patients UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Trimble CL, et al. Cancer 2006; 106: 812-819 Endometrial Hyperplasia • Study of relevance of “qualifying comments” – “cannot exclude a more severe lesion” • Risk of cancer in hysterectomy: – Non-qualified: 37.5% – Qualified: 60% OR: 4,7, p = 0.03 • Summary: findings may vary depending on additional comments • Separate studies: intraoperative frozen section may be useful UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Miller C, et al. Am J Obstet Gynecol 2008; 199(1):69.e1-4 Atypical Hyperplasia: Staging? • Due to high risk of cancer: stage all? • 67 patients with AH underwent node dissection (additional 21 unstaged) – Cancer at hysterectomy: 28% (25 patients) – Surgical outcome same in staged vs unstaged No additional morbidity • Node dissection influenced management in 7 of the 25 patients (28%) • Summary: node dissection should be considered UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Whyte JS, et al. Am J Obstet Gynecol 2010; 202(2):176.e1-4 UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Hyperplasia: EIN • Endometrial Collaborative Group – self-convened group of gynecologic pathologists – discussion of diagnosis and management of premalignant disease • reason: improve diagnostic accuracy – standardization • background: data supports clonal basis of premalignant disease UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology EIN • computerized morphometric analysis • architectural features: – epithelial crowding displaces stroma – Key: VPS < 55% single best predictive value • nuclear features also included • attempt to develop standardized features for diagnosis • validated with clonal and clinical studies • database of referenced tissues available on Web – www.endometrium.org UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology EIN: Classification • EH: endometrial hyperplasia – disordered proliferative through complex hyperplasia – not premalignant • EIN: endometrial intraepithelial neoplasia – true neoplasm; premalignant – single category subdivision: not reproducible, prognostic – still potentially difficult to distinguish from carcinoma but can distinguish from non-premalignant UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Morphometry Baak, et al. (2005) • Multicenter trial; 477 patients • Compared WHO 1994 criteria to EIN • WHO: – 13% of AH progressed – 2.3% of non-AH progressed • EIN: – 19% of EIN progressed – 0.6% of non-EIN progressed UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Baak JP, et al. Cancer 2005; 103: 2304-2312 Morphometry Baak, et al. (2005) • Sensitivity for detecting premalignant lesions: – EIN: 92% – WHO: 67% (all atypical hyperplasias) – Complex atypical hyperplasia alone: 46% • Regression analysis: – EIN was strongest prognostic index of future carcinoma UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Baak JP, et al. Cancer 2005; 103: 2304-2312 Morphometry • Baak, et al (2002): – OR for carcinoma based on D-score: 115 • BUT: studies of computer-based system – requires equipment, training – can be applied subjectively (??) Mutter: subjective vs computer-based morphometry κ: 0.69 not studied UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Morphometry: Summary • needs further study – initial data compelling • WHO incorporating into guide • potential management applications – Netherlands: D-score > 1: progestin, follow EMS D-score >0, < 1: progestin; repeat sample, D-score D-score < 0: hysterectomy Cost savings: $8M per year average avoiding unnecessary hysterectomy UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Micropapillary Tumors • pathology: delicate fine branching papillae – arise directly from thick papillae – must be > 5 mm, otherwise APT • implants: more frequent – 44 cases: 55% invasive (6% - 9% for APT) • prognosis: – 5 year survival: 84% – 10 year survival: 58% – recurrence of cancer: 35% with advanced stage micropapillary UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Micropapillary Tumors • bilateral: 64% • Stage: – Stage 1: 45% – Stage 2: 18% – Stage 3: 37% 55% Stage 2/3 for serous: 40% • surface involvement: 54% (>> APT) UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Serous APT: Facts • extraovarian “disease”: 40% – endosalpingiosis: 40% – APT implants: 40% noninvasive: 31% invasive: 9% – unilateral: 15% > Stage 1; bilateral: 56% > Stage 1 • survival: Stage 1, > 2000 pts, 6.7 year follow-up: 99.5% • microinvasion: 1.3% - 10% – prognosis: 94 pts, 7 year follow-up: 100% UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Implants - Problems • incidence, survival vary • biopsies often superficial • definitions vary – strict: not as common only true invasion: infiltration into underlying tissue – less stringent: more common less effect on survival – if relax criteria, less significance in prognosis • small number of patients UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Implants and Nodes • types: – noninvasive: epithelial desmoplastic – invasive: • survival (89 month follow-up) – noninvasive: 95.3% – invasive: 66% • nodes: rare with APT (63 total cases) – 43 pts with + nodes, 6.5 year follow-up: 98% survival UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Placental Reports: Exaggerated Placental Site • “exhuberant” proliferation of normal implantation site intermediate trophoblast – Considered a normal variant • Normal pregnancies or abortion • Preserves normal placental site architecture • Main DDx: PSTT UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Placental Reports: Placental Site Nodule • Well-circumscribed aggregates of chorionic (not implantation site) intermediate trophoblast – Key: hyalinized stroma – Immunohistochemistry correlates with chorionic trophoblast • Etiology: formerly involuted placenta – Now considered benign counterpart to ETT • DDx: PSTT, exaggerated placental site, SCC (cervix) UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology Placental Reports: Placental Site Nodule • Many patients have had prior EAB or C-S • Most often incidental findings – Evaluation of abnormal Paps; AUB – May be multiple – May occur in cervix (up to 40%) or tube • Antecedent pregnancy: 2 – 108 months • Non-neoplastic: no further treatment needed UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology UNIFORMED SERVICES UNIVERSITY of the Health Sciences Department of Obstetrics and Gynecology