postmenopausal endometrium

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POSTMENOPAUSAL ENDOMETRIUM Dr. Sharda Jain Director: Global Institute of Gynaecoloy at Pushpanjali Crosslay Hospital Secretary general: Delhi Gynaecologist Forum

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POSTMENOPAUSAL ENDOMETRIUM. Dr. Sharda Jain Director: Global Institute of Gynaecoloy at Pushpanjali Crosslay Hospital Secretary general: Delhi Gynaecologist Forum. Learning objectives. Menopause Normal Postmenopausal Endometrium Pathophysiology: before & after menopause - PowerPoint PPT Presentation

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Page 1: POSTMENOPAUSAL      ENDOMETRIUM

POSTMENOPAUSAL ENDOMETRIUM

Dr. Sharda JainDirector: Global Institute of Gynaecoloy at Pushpanjali

Crosslay HospitalSecretary general: Delhi

Gynaecologist Forum

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Learning objectives• Menopause • Normal Postmenopausal Endometrium • Pathophysiology: before & after menopause • What warrants investigations • Case Studies• Endomtrial evaluation • Personal Experience• Review of Literature

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•AFTER 12 MONTHS' SPONTANEOUS AMENORRHOEA.

•FSH >30

Menopause

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Postmenopausal Endometrium

No more than thin line

2.3 mm ± 1.8 mm(0-10)

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PRIOR TO MENOPAUSE:• Short cycle (↓ proliferative)

• ↑ Moderate Elevation of FSH

• Anovulation – Unapposed oest

- DUB

- Hyperplastic endo.

PATHOPHYSIOLOGY

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PATHOPHYSIOLOGYOnce menopause occurs, oestrogen and progesterone are no longer produced by the ovaries; nor are they produced in any appreciable amounts by the liver and fat.

The endometrium regresses to some degree, and no further bleeding should occur.

If bleeding does resume - endometrium must be evaluated.

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AMENORRHEIC + NO HORMONE THERAPY 4.0SEQUENTIAL HORMONE THERAPY (DAY 5) 4.0ESTROGEN ALONE/COMBINED ESTROGEN 5.5WITH PROGESTERONETIBOLONE 5.5RALOXIFENE 4.0

TAMOXIFEN 8.0

HYPERTENSIVE ON MEDICATION 6.5

Norms for Endometrial Thickness inPostmenopausal Women (MM)

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WHAT WARRANTS

INVESTIGATION

AND EVALUATION?

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Fluid - Anachoic area ↑ Endometrium – Warrants investigation

Thick Endometrium

NO POST MENOPAUSAL BLEEDING

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POST MENOPAUSAL BLEEDING

• PRECANCEROUS / CANCER of cervix & uterus• Benign conditions – eg. Polyp

• Chronic endometritis- eg. TB• Disorders of coagulation/ Blood dyscrasias

• Systemic Disease- eg. Hypertension • Drugs – anticoagulants, Tamoxiphen.

Herbal drugs, HRT

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Postmenopausal Bleeding

• Benign conditions are most frequent causes of PMB but endometrial cancer is the most serious potential underlying cause

• One Should think endo. Ca untill proven otherwise.

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75% of women with endometrial cancer

are postmenopausal.

RISK ASSESSMENT

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RISK FACTORS FOR ENDOMETRIAL CANCER

are conditions typically associated with chronic elevations of endogenous estrogen levels or increased estrogen action at the level of the endometrium. These include

OBESITY. HISTORY OF CHRONIC ANOVULATION. DIABETES MELLITUS. ESTROGEN-SECRETING TUMORS. EXOGENOUS ESTROGEN UNOPPOSED BY PROGESTERONE . TAMOXIFEN USE. A FAMILY HISTORY OF LYNCH TYPE II SYNDROME

(HEREDITARY NONPOLYPOSIS COLORECTAL, OVARIAN, OR ENDOMETRIAL CANCER).

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Systemic conditionsAbnormalities of the hematologic system

also must be considered as a possible cause of postmenopausal bleeding.

On rare occasions, AUB will be the first sign of leukemia or a blood dyscrasia.

Overuse of anticoagulant medications such as aspirin, heparin, and warfarin-which are taken with greater frequency by patients in this age group-may contribute to postmenopausal bleeding.

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POSTMENOPAUSAL BLEEDING &

HRT • The occurrence of uterine bleeding or

spotting after the initiation of HRT is not unusual. More than half of HRT users will have some spotting or bleeding at the beginning of therapy.

• Usually such bleeding is lighter than a menstrual period and lessens with time; after 6 months, it stops completely in most women.

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ENDOMETRIAL EVALUATION IS CALLED FOR WHEN :

1. any menopausal woman not taking HRT develops uterine bleeding after more than 1 year of amenorrhea.

2. any postmenopausal woman on HRT for 6 months or more with persistent uterine bleeding.

3. and any previously amenorrheic woman on HRT who begins bleeding without apparent cause.

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CASE STUDY - 164 years old G2 P2 : 16 years postmenopausal

• Went to physician for pain in abdomen• Ultrasound revealed18 mm endometrial strip• No discharge/ No Bleeding, 70 kg, BMI - 32• Mild hypert, DM controlled.

• EB – Well differentiated Adeno Carcinoma • Staging laparotmy and pan hysterectomy

• IA- Disease

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68 years• Menopausal 20 years• 3 episodes of bleeding in last 6 weeks• Hypertension/ diabetic/ obese/ BMI-31• TVS – Uterus bulky for age. Endometrial strip is 18

mm. • Office E.B. well differentiated adeno-carcinoma• 1 A disease

CASE STUDY-2

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54 years, professor in DU

• Menopause = 48 years

• Single episode of spotting on 13/8/2010

• TVS – 7-8 mm

• HPE – Clear all Endo. Ca.

CASE STUDY - 3

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CASE STUDY - 4• 54 year old G2 P2• Had HRT at age 50 for Hot flushes – 6 months• Presented with 3 episodes of vaginal bleeding over last 6 weeks (3 years after

menopause)• TVS show endometrial strip of 12 mm, Uterus- normal in size.

• E.B. proliferative endometrium• Hysteroscopy normal …. Spotting for 3 months

• Refused Hysterectomy

Uterine Balloon Therapy

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60 YEARS, UNMARRIED PROFESSOR• Menopause – 48 years

• 52 years – Heavy Bleeding

• Ultrasound – 3-4 mm Endo. Strip

• D&C /Hysterectomy – Simple hyperplasia

of endometrium

- Refused Hysterectomy

Uterine Balloon Therapy

CASE STUDY - 5

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CASE STUDY-656 years multi gravida Pain in lower abdomen + ; No Postmenopausal Bleeding • Appears well• BMI < 25, 60 kg• Normotensive• General exam unremarkable• Speculum: CERVICAL POLYP• Ultrasound - Uterus normal, endometrium 12 mm, Both

ovaries normal• INFLAMMATORY POLYP AND TUBERCULAR

ENDOMETRITIS

ATT Given - EB &- Hysteroscopy

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THE DURATION OR AMOUNT (STAINING VS GROSS) OF BLEEDING DOES NOT MAKE ANY DIFFERENCE.

IT GIVES NO CLUE TO DIAG.

SAME IS TRUE FOR ENDOMETRIAL THICKNESS.

RISK ASSESSMENT

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• Vaginal ultrasonography.

• Saline infusion sonography (Hydrosonography)

• Office Endometrial biopsy.

• Conventional F/C or D/C

• Hysteroscopic guided biopsy.

DIAGNOSTIC TOOLS

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Sensitivity and specificity are often used to summarise the performance of a diagnostic test.

Sensitivity is the probability of testing positive if the disease is truly present.

Specificity is the probability of testing negative if the disease is truly absent.

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VAGINAL ULTRASOUND

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Although the test is very specific , it isn't sensitive. Many women without endometrial cancer will have an endometrial thickness of 4 mm or more

VAGINAL ULTRASOUND

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A CUT-OFF THRESHOLD OF 3 MM

OR 5MM ?cut-off point of 3 mm is less likely to

miss cancer than cut-offs of 5 mm.

But unfortunately a lower cut-off means a greater proportion of women requiring invasive investigation.

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THE PATIENT RISK GROUP

•Low pre-test probability•On HRT•On tamoxifen therapy

• High pre-test Probability (high risk)

Cut off threshold 5mm Cut off threshold 3mm

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Endometrial polyp in hyperechoic thickened endometrium

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The introduction of intrauterine fluid (saline-infusion sonography) during transvaginal ultrasound is one of the most significant advances in ultrasonography of the past decade.

SALINE – INFUSION SONOGRAPHY

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Uterine fibroids and adenomyomas generally are apparent on ultrasound. Uterine polyps may appear as a thickened endometrial stripe, but these and submucous myomas can be clearly identified as filling defects when a SIS is performed

SALINE – INFUSION SONOGRAPHY (SIS)

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At transvaginal ultrasonography , the finding of a thickened central endometrial complex, with or without cystic changes, is often

nonspecific.

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The Thickened endometrium may be a polyp

With polyps the endometrial-myometrialinterface is preserved

CYST

POLYP

well-defined, homogeneous,isoechoic to the endometrium

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The Thickened endometrium

may be a polyp

With polyps the endometrial-myometrialinterface is preserved

POLYPcatheter

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• Office Endometrial Biopsy

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A useful suction endomtrial sampling (Probet) with 3.1 mm in outside diameter and no pump or syringe

required.

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An endometrial suction sampling with syringe vacuum

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SAMPLING OF THE ENDOMETRIUM

• OFFICE BIOPSY PROCEDURE (Probet Endometrial Curette, Vabra aspirator, Karman cannula) will agree with a D&C under GA ~95% of the time

• Office biopsy has a 16% false negative rate when the lesion is a polyp or the cancer covering less than 5% of the endometrium– Guido et al. J Reprod Med. 1995;40:553

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Preoperative D&C will agree with diagnosis at hysterectomy - 95% of the time

The role today of the formal D&C or F/C probably is very limited because the diagnosis usually can be made in the office by endometrial biopsy (95%).

DILATATION AND CURETTAGE

“Gold STANDARD”

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Hysteroscopic visualization has several advantages:

immediate office evaluation, visualization of the endometrium and

endocervix, the ability to detect minute focal

endometrial pathology and to perform directed endometrial biopsies.

OFFICE HYSTEROSCOPIC-DIRECTED BIOPSY

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ACOG/ CANADIAN (SOGC) WHAT TO DO?

CLINICAL PRACTICE GUIDELINES

2000• Endometrium ≥ 4, even if No bleeding

• Abnormal vaginal bleeding after menopause

↓• Endometrial Cancer must be ruled out

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A SYSTEMATIC REVIEW OF 90 STUDIES AND META-

ANALYSIS

ENDOMETRIAL THICKNESS MEASUREMENT FOR DETECTING

ENDOMETRIAL CANCER IN WOMENWITH POSTMENOPAUSAL

BLEEDINg: Opmeer BC, Khan KS et.al (Obstet Gyneol 2010;116:160-7)

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Meta analysis 90 Studies of POST MENOPAUSAL BLEEDING

• OVERESTIMATED THE DIAGNOSTIC ACCURACY OF ENDOMETRIUM THICKNESS

• CRITICAL THICKNESS – 3 MM TO R/O ENDOMETRIAL CARCINOMA

Opmeer & KanObsted Gynee 2020

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CRITICAL THICKNESS – 3 mm

•unexplained

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No Bleeding TVS

Endometrial

thickness is > 3mm

If low risk

office endometrialbiopsy and SIS

If high risk

D/C biopsy ORHysteroscopy

Or both

fail to do If

Endometrialthickness is < 3mm

follow

But symptoms persist

IN WOMEN WITH CONTINUED BLEEDING AFTER A NEGATIVE INITIAL EVALUATION, FURTHER TESTING

WITH HYSTEROSCOPICALLY DIRECTED BIOPSY IS ESSENTIAL,

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Unsatisfactory, unable to do

Low Risk for Ca High Risk for Ca D&C (D&C + hysteroscopy) ± Hysteroscopy

Post Menopausal Bleeding TVS

Office Endometrial Biopsy

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POST MENOPAUSAL BLEEDING (Our Experience)

Etiology %

Atrophic Endometrium 31

Endo. Hyperplasia (simple complex, atypical)

26

Endometrial Ca. 14

Polyp endo/ cervical 6

Proliferative Endo (Exogenous Estrogen)

1

Total (Jan 2007 – till date) 78

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Post Menopausal Endometrium

Endometrium (mm)

Number of Patient

Details

<5 32 Atrophic-31, Cancer-1

<10 16 Cervical Polyp- 3, Endo. Polyp-3, Cancer – 1, Simple Hyperplasia-9,

>10 30 Carcinoma- = 12 Submucous fibroid-1, Simple hyperplasia - 14 Complex hyperplasia-2 Atypical = 1

Total 78

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NORMAL ENDOMETRIUM

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ENDOMETRIAL POLYP

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POLYP AND ATYPICAL HYPERPLASIA

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ENDOMETRIAL CANCER:TRANSVAGINAL ULTRASOUND SCREENING

< 5 mm Endo strip also showed CA.

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ENDOMETRIAL CANCER:TRANSVAGINAL ULTRASOUND SCREENING

6 – 10 mm Endo strip also showed CA.

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ENDOMETRIAL CANCER:TRANSVAGINAL ULTRASOUND SCREENING

Fluid

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Endometrium: Post-menopausal atrophy

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ENDOMETRIAL SIMPLE HYPERLASIA

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ENDOMETRIAL HYPERLASIA - COMPLEX

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ENDOMETRIAL HYPERPLASIA - ATYPICAL

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GRADE 1 ENDOMETROID CARCINOMA

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GRADE 3 ENDOMETROID CARCINOMA

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ENDOMETRIAL CARCINOMA: POOR PROGNOSIS CELL TYPES - PAPILLARY SEROUS

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ENDOMETRIAL CARCINOMA - POOR PROGNOSIS CELL TYPES CLEAR CELL

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