Menopause Lecture Notes Fall 2024 PDF

Summary

These lecture notes cover menopause, discussing symptoms, risks, benefits of hormone therapy, and non-hormonal options for treatment. The document also details the critical window hypothesis and important factors to consider when deciding on a treatment approach.

Full Transcript

Menopause
SHERYL MATHE W, PHARMD, BCPS
PHAR508, FALL 2024

S L I D ES A D A P T E D F R O M L O U I S E PA R E N T - S T E V E N S , P H A R M D , B C P S
Goals and Objectives
Identify the symptoms of menopause

Identify the risks versus benefits of hormone therapy for menopause

List the non-hormonal options for the management of menopausal
symptoms

Develop a patient-specific treatment plan for the management of
menopausal symptoms
Required Reading
Pharmacotherapy (DiPiro) 12th ed
Chapter 102: Post Menopausal Hormone Therapy

Additional materials posted on Blackboard
Table 1: Risks and Benefits of HT
Table 2: Agents used for postmenopausal HT
Table 3: Example ET/EPT regimens and expected vaginal bleeding patterns
What is Menopause?
A natural life event → not a disease

Permanent cessation of menses, following the loss of ovarian follicular function
Decreased production of sex hormones (estrogen, progestin)

Stages of natural menopause:
Perimenopause
Menopause (amenorrhea >12 months)
Postmenopause (1 year after menopause and beyond)

Induced menopause → due to removal of ovaries or ablation of ovarian function
Epidemiology
Median age of onset in the US = 51 years (can vary from 40-58 years)
Onset before age 40 = premature ovarian insufficiency (POI)

Women are spending nearly 40% of their lives in post-menopause

~6,000 women in the US reach menopause everyday
Clinical Presentation
Vasomotor symptoms
AKA hot flashes, night sweats (diurnal pattern)
Develop in up to 80% of women and last ~7.5 years on average
Wane with time since menopause
Sudden feeling of warmth and increased sweating/flushing
Severity, duration, and frequency vary from woman to woman
25% of women experience severe vasomotor symptoms
Clinical Presentation
Genitourinary Syndrome of Menopause (GSM)

Vaginal atrophy
Thinning, drying, and inflammation of vaginal walls
Dyspareunia (painful intercourse)

Urinary symptoms
Urinary urgency, dysuria
Recurrent UTI
Clinical Presentation
Psychological symptoms
Increased risk of depression
Mood changes
Poor concentration and memory (reach premenopausal levels again after menopause)
Decreased libido
Insomnia and fatigue (due to nocturnal hot flashes)

Breast atrophy
Due to decrease in estrogen
Clinical Presentation
Increased risk of osteoporosis
Estrogen is essential for bone growth
Major cause of morbidity in post-menopausal women

Increased risk of CV disease?
#1 cause of death in post-menopausal women
Menopause associated with more adverse lipid profile
Diagnosis
No menses for one year
In absence of other causes for amenorrhea

Diagnosis typically retrospective

Elevated FSH levels (> 40)
Management
Goals of therapy:
Relieve symptoms
Improve quality of life
Minimize adverse effects

Treatment should be individualized

Important Terms:
HT = hormone therapy
MHT = menopausal hormone therapy
ET = estrogen therapy
EPT = estrogen progesterone therapy
Guidelines
Numerous guidelines available
◦ NAMS: 2023 Nonhormone Therapy Position Statement
https://menopause.org/wp-content/uploads/professional/2023-nonhormone-therapy-position-
statement.pdf
◦ NAMS: 2022 Hormone Therapy Position Statement
https://www.menopause.org/docs/default-source/professional/nams-2022-hormone-therapy-position-
statement.pdf
◦ AACE: The 2017 Menopause Position Statement Updated
https://journals.aace.com/doi/pdf/10.4158/EP171828.PS
◦ NAMS: 2020 Genitourinary Syndrome of Menopause Position
Statement
https://journals.lww.com/menopausejournal/Fulltext/2020/09000/The_2020_genitourinary_syndrome
_of_menopause.5.aspx
Non-Pharmacologic Management
Hot flash trigger avoidance
Wear layered clothing
Lower room temperature
Decrease intake of spicy foods, caffeine, hot beverages
Regular exercise
Aerobic (CV protection) and weight-bearing (bone protection)
Diet
Heart-healthy
Adequate calcium and Vitamin D
Pharmacotherapy
Hormone therapy
Estrogen +/- progestin
Tissue selective estrogen complex (TSEC)
SERMs

Non-hormonal therapy
Serotonergic agents (SSRI/SNRI)
NK3R antagonist
Antiepileptic drugs
Antihypertensives
Local (vaginal) therapies
Hormone Therapy
 HORMONE THERAPY (HT)

ESTROGEN ONLY (ET) ESTROGEN +
PROGESTERONE
(EPT)
Systemic Estrogen Localized Estrogen (oral, transdermal,
(oral, transdermal, (low-dose vaginal) high-dose vaginal)
high-dose vaginal)

ESTROGEN +
BAZEDOXEFINE
(oral)
Estrogen Therapy (ET)
Systemic estrogen monotherapy
FDA-approved indications:
Vasomotor symptoms
Genitourinary symptoms (GSM)
Premature hypoestrogenism
Prevention of bone loss
For use in women without a uterus
Increases risk of endometrial cancer if used in women with a uterus
Estrogen-Progestin Therapy (EPT)
Systemic estrogen-progestin therapy
For use in women with intact uterus
Uterine protection is the only reason to add progestin component to ET
Estrogen + Bazedoxifene (Duavee)
Systemic (oral) estrogen + SERM = TSEC (tissue-selective estrogen
complex)
Bazedoxefine = estrogenic in bone, antiestrogenic in uterus/breast
Indication (in women with uterus):
Moderate-severe vasomotor symptoms
Prevention of postmenopausal osteoporosis
Advantage: do not need to add a progestin component
Same risks/contraindications as ET
Localized Estrogen Therapy (ET)
Vaginally administered low-dose estrogen that does not result in clinically
significant systemic absorption

Indication: menopausal vaginal atrophy

Does NOT require concomitant progestin therapy (even if a woman has a uterus)

Therapeutic response typically after 2 weeks of daily use
Maintenance dosing typically 2-3x weekly
Risks versus Benefits of
Hormone Therapy
Women’s Health Initiative (WHI)
Randomized, double-blind, placebo-controlled trial (1991)
To evaluate effects of MHT on heart disease, osteoporosis, cancer in women aged 50-79 years
(mean age 63.5 years)
Two arms:
Estrogen + progestin (in women with an intact uterus) – n=16,608
Estrogen alone (in women with history of hysterectomy) – n=10,739

Primary outcome: incidence of coronary heart disease (CHD)
Primary safety outcome: invasive breast cancer
Other outcomes studied included: stroke, PE, endometrial cancer, colorectal cancer, hip fracture,
and death due to other causes
WHI Results
Estrogen + progestin arm terminated early (5.6 years) due to increased breast
cancer risk and unfavorable risk-benefit ratio
Estrogen only arm terminated early (7.2 years) due to increased stroke incidence

Key takeaways:
Dramatic reduction in MHT prescriptions after results were published in 2002
Only studied one dose and formulation
Important to note that it was an older population (average age 63 years), on average ~12
years past menopause
Subsequent subanalyses of the WHI and other studies have shown that younger
women/closer to menopause had a more beneficial risk-benefit ratio
Importance of Timing
Critical window hypothesis = effects of HT depend on the timing of initiation with
respect to age and/or onset of menopause, with benefits limited to early initiation

Early use:
< 10 years since menopause and < 60 years old at initiation
No change or decreased risk of CHD
Late use
> 10 years since menopause and > 60 years old at initiation
Increased risk of CHD, stroke, and VTE

Overall, HT should not be used for chronic disease prevention, but is a reasonable
option for managing menopausal symptoms
Established Benefits
Vasomotor symptoms
Osteoporosis
Reduced risk of hip, spine, and wrist fractures
Protective effect does not persist after cessation of treatment
Vaginal atrophy
Established Risks
Thromboembolic disease
Breast cancer
Cardiovascular disease
Endometrial cancer
Ischemic stroke
Gallbladder disease
Hypertriglyceridemia
Absolute Contraindications for HT
Venous
Undiagnosed Severe active liver thromboembolism
vaginal bleeding disease
(VTE)

High risk of
History of CHD or
thromboembolic History of stroke
MI
disease

Personal history of
breast,
endometrial, or
ovarian cancer
Absolute Contraindications
In women with absolute contraindications to systemic estrogen, localized low-
dose vaginal estrogen may be acceptable
Relative Contraindications
Use cautiously, monitor closely!
Endometriosis or uterine fibroids
Gallbladder disease or moderate liver disease
Hypertriglyceridemia
Migraines
Uncontrolled DM or HTN
Obesity
Age >60 years or >10 years since menopause (at initiation)
Strong family history of breast or ovarian cancer
Current tobacco use
Product Selection and
Dosing for HT
Product Selection
Start with the lowest effective dose for symptom control
Fewer adverse effects and better overall benefit-risk profile

Various routes available (oral, transdermal, topical, intravaginal,
intramuscular)

Use transdermal route in patients with:
Increased risk of VTE
Gallbladder disease
HTN
Hypertriglyceridemia
Product Selection
Patients with a uterus must use combination EPT (for systemic HT)

Can use separate estrogen and progestin products, or combination products

Preferred progestin is micronized progesterone
EPT Dosing Regimens
Variety of dosing regimens available
Continuous cyclic EPT – estrogen administered daily, progestin coadministered 12-14 days of
28 day cycle
Scheduled withdrawal bleeding in ~90% of women
Continuous combined EPT (preferred) – can use oral or transdermal preparations, or
administer systemic estrogen + levonorgestrel IUD
Absence of withdrawal bleeding (after 1 year for majority of patients)

Patients should be counseled about potential for bleeding
Patient should be involved in selection of regimen
Resumption of bleeding does not indicate return of fertility
Adverse Effects of Systemic HT
Nausea
Breast tenderness
Headaches
*Side effects often diminish with
Increased BP continued use

Leg cramps *If persistent, try dose adjustment
Mood swings or change in product

Decreased libido
Skin irritation (with transdermal products)
Localized Low-Dose Vaginal ET
◦Indicated for vaginal atrophy
◦Limited systemic absorption occurs—may be okay to use
in women with absolute CI
◦No proven systemic benefits
◦Does not require concurrent progestin use
◦Products
◦ Low dose vaginal ring (7.5mcg/day of estradiol)
◦ Cream/Tablets (conjugated estrogens, estradiol
estropipate)
Place in Therapy for ET/EPT
Post-menopausal women with vasomotor symptoms
Safety profile most favorable in healthy women