Menopause Management.Tiffany Weber€¦ · Management of menopausal symptoms. N Engl J Med 2006;...

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©UNIVERSITY OF UTAH HEALTH, 2017 Menopause Management Tiffany Weber, MD Assistant Professor University of Utah OB/GYN Department

Transcript of Menopause Management.Tiffany Weber€¦ · Management of menopausal symptoms. N Engl J Med 2006;...

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Menopause Management

TiffanyWeber,MDAssistantProfessor

UniversityofUtahOB/GYNDepartment

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DISCLOSURES

• No financial disclosures

• I have not yet experienced menopause

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HISTORY OF MENOPAUSE

• Described by Aristotle, but not defined until 1820s• AKA “hysteria”

• Wide variety of treatments: opium, cannibus, ground up animals ovaries, “testicular juice”, vaginal solutions, oophorectomy, hysterectomy, clitoridectomy

• 1930s, estrogen and progesterone identified and a more medical understanding of menopause began to develop

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MENOPAUSE BACKGROUND

• Women spend about 1/3 of their life after menopause

• “Grandmother hypothesis”

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MENOPAUSE DEFINITION

• Definition: permanent cessation of menstruation

• Median age in the US is 51 years

• Due to loss of ovarian function

Drashrafsabry.com

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Drugs.com

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ESTROGEN

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MENOPAUSE: HORMONES

• Estradiol

• Progesterone

• FSH

• Androgens

embryology.med.unsw.edu.au

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MENOPAUSE

• Amenorrhea• Vasomotor symptoms• Dyspareunia• Sleep Disturbance• Weight redistribution• Mood lability

• Osteoporosis• Vaginal atrophy• Urinary incontinence• Heart disease• Poor skin elasticity, muscle

tone• Cognitive changes?

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TREATMENT

• YES• Vasomotor symptoms• Osteoporosis• Vaginal atrophy

• NO• Weight gain• Cognitive changes• Heart Disease

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VASOMOTOR SYMPTOMS

• Of women with hot flushes:– 87% of women who experience these symptoms experience on a

daily basis– 33% have more than 10 episodes per day– How long do these symptoms last?

• WHO KNOWS! (reported 6 months to 10 years)

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VASOMOTOR SYMPTOMS TREATMENT

• GOLD STANDARD: Systemic estrogen • Low dose • Decreases frequency and severity of hot

flushes

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VASOMOTOR SYMPTOM TREATMENT-NONHORMONAL

• Lifestyle changes

• Supplements

• Paxil (only FDA approved non hormonal treatment)

• Clonodine

• Gabapentin

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VASOMOTOR SYMPTOMS AFTER HRT

• 50% of women have vasomotor symptoms return

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OSTEOPOROSIS

• WHI statistically significant reduction with HRT• 33-36% reduced risk of hip and vertebral fractures with ET or

Combined ET/PT• HRT approved for prevention of osteoporosis• Benefit is dose related• Bone mineral density due to HRT is lost within 1-2 years after

discontinuing treatment (so may need to transition to alternate treatment)

ACOG Practice Bulletin “Osteoporosis”

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VAGINAL ATROPHY (GENITOURINARY SYNDROME OF MENOPAUSE)

• Symptoms: dyspareunia, vaginal dryness, discharge, itching

• Due to: loss of superficial epithelial cells, decreased subcutaneous fat, tissue is fragile

uptodate

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VAGINAL ATROPHY TREATMENT

• Lubricants/moisturizers• Estrogen

– Local (cream, ring or tablet)– Systemic

• Ospemifene• Vaginal dilators

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WEIGHT GAIN

• Cochrane review:• No difference in weight gain, BMI

– Unopposed estrogen– Combined estrogen and progesterone– Non-HRT users

• Insufficient data for: fat distribution, waist hip ratio

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COGNITIVE CHANGES

• SWANS, Nurses Health Study and WHI:• Does not support decline in cognitive function• Increase in anxiety and depression which are

independent risk factors for negative cognitive changes• Dementia risk

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INITIATING HRT

• What to start?• When to start?• How to discuss risks with patient

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HORMONE REPLACEMENT THERAPY

• Estrogen• Progesterone• Testosterone

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ESTROGEN REPLACEMENT THERAPY

• Systemic– Oral, transdermal (patch, gel, sprays)

• Vaginal

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ESTROGEN REPLACEMENT THERAPY

• Low dose– 0.3-0.45mg/d oral conjugated equine estrogen– 0.5mg/d oral micronized estradiol– 5mcg/d oral ethinyl estradiol– 0.025-0.075mg/wk of transdermal estradiol patch

• Other topicals: gels, creams, spray

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VAGINAL ESTROGEN

• Do not need progestin treatment• Cochrane metanalysis: vaginal estrogen not associated

with increased risk for endometrial hyperplasia• No endometrial surveillance required in asymptomatic

women

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VAGINAL ESTROGEN AND HISTORY OF BREAST CANCER

• Non-hormonal approaches are the first line choice• Symptoms often worsened by anti-estrogen treatments• RISK VS BENEFIT• Several studies have shown low dose vaginal estrogen have minimal

systemic absorption– Systemic levels do not exceed the normal menopausal range (cream has

greater variability compared to ring or tablet)

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PROGESTIN REPLACEMENT THERAPY

• NECESSARY if they have a uterus to prevent endometrial hyperplasia

• May help vasomotor symptoms• Safety? No great studies looking at unopposed progestin

use

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TESTOSTERONE REPLACEMENT THERAPY

• No benefit for vasomotor symptoms• May improve sexual function and number of satisfying

sexual episodes

• Risks: – dyslipidemia– clitoromegaly, hirsutism, acne, hair loss

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HORMONE REPLACEMENT THERAPY

• RISKS

– THROMBOEMBOLIC DISEASE

– BREAST CANCER

– HEART DISEASE?

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HRT AND THROMBOEMBOLIC RISK

• Oral Estrogen – 1.2-1.5 fold increased risk of VTE

• Risk per 100,000– 40s: 54– 50s: 62-122– 70s: 300-400– 80s: 700

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HRT AND THROMBOEMBOLIC RISK

• Transdermal estrogens – little or no effect in elevating prothrombotic substances

• The estrogen and thromboembolism risk study (Case control)– OR oral: 4.2, transdermal: 0.9

• Progestins– natural progesterone no increased risk– synthetic progestins increased risk

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HRT AND THROMBOEMBOLIC RISK

• WHI– 41% increase risk of stroke

• 21 to 29 per 10,000 woman-years– These risks were noticed within 1-2 years of initiation

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HRT AND THROMBOEMBOLIC RISK

• Cochrane review

Stroke VTE PE

AbsoluteRiskIncrease per1000

6 8 4

NNTH 165 118 242

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HRT AND BREAST CANCER RISK

• Collaborative Group on Hormonal Factors in Breast Cancer:– 52,705 women with BC, 108,411 women without

breast cancer– Each year a women uses HRT, risk of BC

increases 2.3% (did not differentiate between ET and ET/PT)

• WHI– in ET/PT there were 8 excess cases per 10,000

women years– No statistical difference between placebo and

ET

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HRT AND HEART DISEASE

• WHI study terminated early due to cardiovascular events (and worsened global index)

• 29% increase in cardiovascular events – but no significant difference in CHD deaths

• 30/10,000 woman-years to 37/10,000 woman-years

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HRT AND HEART DISEASE

• “Timing hypothesis”• WHI:Average age of participants was 63• Subsequent WHI analysis:• Women age 51-59 showed reduced total mortality

(decreased 30%) with HRT within the first 10 years after menopause

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HRT AND HEART DISEASE

• Timing hypothesis (RE-EVAL of WHI)– 1000 women under 60 years old start HRT:– 6 fewer deaths– 8 fewer cases of CHD– 5 additional VTE

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HRT AND HEART DISEASE

• Cochrane review subanalysis

• Timing theory (<10 years from menopause)– Increased risk of VTE– Lower mortality– Lower CHD– No statistical significance on stroke

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HRT AND HEART DISEASE

• Heart and Estrogen/Progestin Replacement Study (HERS) and follow up (HERSII)– RCT: conjugated equine estrogen and medroxyprogesterone

acetate– CHD risk among women with CHD

• Tx group: 52% increase in CHD events in the 1st year

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HRT AND HEART DISEASE

• HRT should not be used for primary or secondary cardiac disease prevention

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HRT AND THE PATIENT

• Know the benefits for the patient

• Discuss the risks for the patient

• Determine the goals of treatment with the patient

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BIG PICTURE IDEAS

• Do use HRT for treatment for vasomotor symptoms (in appropriate patients)– Lowest dose and shortest duration to control

symptoms• Do use HRT for vaginal atrophy• Do NOT use HRT for CV protection• HRT is probably safest when initiated at the

onset of menopause

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REFERENCES

• Management of menopausal symptoms. ACOG Practice Bulletin #141, January 2014.• Compounded bioidentical menopausal hormone therapy. ACOG Committee Opinion #532, Aug 2012• The use of vaginal estrogen in women with a history of estrogen-dependent breast cancer. ACOG Committee Opinion #659, March 2016.• Postmenopausal Estrogen Therapy: route of administration and risk of venous thromboembolism. ACOG Committee Opinion #556. April 2013• Hormone therapyandheart disease. ACOG Committee Opinion #565, June 2013• Kongnyuy,etal. Oestrogen and progestogen hormone replacement therapy for peri-menopausaland post-menopausal women: weight and body fat distribution. Cochrane

database of systematic reviews. 1999, issue 3, Art No CD001018• Dodin, et al. Acupuncture for menopausal hot flushes. Cochranedatabase of systemaitic reviews 2013, issue7, Art No CD 007410• Somboonporn, et al. Testosterone for peri and postmenopausal women. Cochrane database of systematic reviews 2005, Issue 4. Art No CD004509• Boardman, et al. Hormone therapy for preventing cardiovascular disease in postmenopausal women. Cochrane database of systematic reviews 2015, Issue 3. Art No CD002229• Osteoporosis. ACOG Practice Bulletin #129. Sept 2012• Grady D. Clinical Practice. Management of menopausal symptoms. N Engl J Med 2006; 355:2338-47.• Castelo-Branch C, et al. Management of post-menopausal vaginal atrophy and atrophic vaginitis. Maturitas 2005;52(suppl 1):S46-52.• MacLennan AH, et al. Oral oestrogen and combined oestrogen/progestogen therapy versus placebo for hot flushes.Cochrane Database of Systemic Reviews 2004, Issue 4, Art.

No: CD002978• Anderson, et al. Effects of conjugated equine estrogen in postmenopausal women with hysterectomy: the Women’s Health Initiative Steering Committee. JAMA 2004;291:1701-12.• Somboonporn, et al Testosterone for peri and postmenopausal women. Cochrane Database of Systematic Reviews 2005, Issue 4, Art No CD004509.• Nelson, et al. Nonhormonal therapies for menopausal hotflashes: systematic review and meta-analysis. JAMA 2006;295:2057-71.• Gattuso, etal Gabapentin’s effects on hot flashes in postmenopausal women: a RCT. Obstet Gynecol 2003;101:337-45