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Abnormal Pap in Pregnancy Alexander Burnett, MD Division Gyn Oncology, UAMS April, 2006.

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Presentation on theme: "Abnormal Pap in Pregnancy Alexander Burnett, MD Division Gyn Oncology, UAMS April, 2006."— Presentation transcript:

1 Abnormal Pap in Pregnancy Alexander Burnett, MD Division Gyn Oncology, UAMS April, 2006

2 Objectives 1. Significance of Pap smears during pregnancy 2. Problems with Pap smears 3. Management of abnormal results 4. Treatment during pregnancy 5. Post-partum evaluation

3 Pap smear is part of prenatal testing  Screening opportunity  Cervical cancer is the most common malignancy detected in pregnancy (1-15/10,000)  Majority of cancer patients are stage I -- 83%  CIS detected in ~1/750 pregnancies

4 Cytology during pregnancy Technique: Cervical brush for LBM Ayre spatula + cytobrush Cotton swab is inadequate Endocervical component absent in 55% of Paps that utilized cotton swabs

5 Pregnancy effects on Pap  0.5% - 3.0% of Paps abnormal  Mimics of HSIL: Degenerated decidual cells Cytotrophoblast Arias-Stella reaction (confuse with adenocarcinoma) Immature reactive metaplasia  Mimics of LSIL:Syncytiotrophoblast Multinucleated cells

6 Management of abnormal Pap  Identical to non-pregnant patient  Indications for colposcopy: HSILLSILASC-H ASCUS + HPV AGUS Suspicion for cancer  ECC is never indicated during pregnancy!

7 Colposcopic challenges  Vaginal laxity  Cervical laxity  Inadequate visualization of TZ  Increased vascularity of cervix  Increased squamous metaplasia

8 Frequency of colposcopy  Recommended each trimester for visual inspection of dysplasia  Inadequate transformation zone will often become adequate with cervical eversion over gestation  “Clearance” for delivery  No need to repeat the Pap smear at each colposcopy

9 Biopsy in pregnancy  Should be performed for suspicion of HSIL or invasive disease  Directed biopsy with immediate application of pressure, silver nitrate, and/or Monsel’s  Safe to perform at any stage in pregnancy  Do not repeat biopsy at later colposcopy unless significant change is seen

10 Cone biopsy  Indicated if biopsy suggests microinvasion  Associated with increased bleeding (> 500 cc in 10%), preterm labor, infection, spontaneous abortion in first trimester.  LEEP can be performed, similar complications reported as cold-knife  ONLY done in surgical suite setting

11 Management of SIL in pregnancy  Pre-invasive disease should not be treated in pregnancy  Repeat colposcopy to follow patient with biopsy if a significant change is noted  Re-evaluate in the post-partum period (at least 6-8 weeks)

12 Cervical cancer in pregnancy  Pregnancy does not appear to significantly alter the course of disease  Management is based on gestational age at time of diagnosis: < 20 weekstreat as non-pregnant > 24 weeksawait fetal viability 20 - 24 weeksindividualize

13 Pre-viable treatment  Early cervix cancer: Radical hysterectomy with nodes Radiation therapy/chemotherapy  Late cervix cancer: Chemoradiation

14 Later pregnancy therapy  Document fetal maturity  Deliver via classical C/S  Radical hysterectomy at time of C/S

15 Planned delay in therapy  Numerous reports of patient opting for delays  Follow closely, increased bleeding risk  Chemotherapy has been utilized in rapidly growing cervix cancers  Outcome generally good, but numbers are small  Deliver via C/S

16 Dysplasia management  Delivery route should be for obstetric indications  Several reports have suggested high rate of regression post-partum, particularly if a vaginal delivery has occurred  6-8 weeks post-partum, reasonable to perform PAP, colposcopy, biopsies and ECC

17 Other management considerations  If colposcopy is difficult or suspicious for HSIL or microinvasion, consider referral to expert colposcopist to determine need for biopsy  Vascular lesions with negative Pap smears, consider referral, close monitoring to determine if this is dysplastic/malignant versus physiologic

18 Condylomas during pregnancy  Can rapidly grow during gestation  Increased risk of trauma at delivery  Increased risk of Respiratory Papillomatosis in offspring. Not prevented by C/S or wart therapy  Treatment: TCA, cryo for small lesions Cautery, LEEP, laser for large areas


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