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Lecture 3 Gender Affirming Medical Therapy Townsend HISTORICAL CONTEXT OF TRANSGENDER HEALTHCARE: Care limited to specialized gender clinics (psychiatry, psychology, sexual medicine, endocrinology) Pathologization of trans identities Reparative therapy Excessive gate-keeping Lengthy assessments prior to treatment Expectation of binary transition BARRIERS TO CARE AND CONSEQUENCES: BARRIERS Prior negative experiences in healthcare settings Fears or expectations of negative experiences Body dysphoria (and clinician discomfort with trans bodies) Lack of provider comfort, knowledge/trans competence CONSEQUENCES Postponing care until problems are more serious Avoidance of care leads to missed screening, untreated health conditions Self-medicating (hormone therapy) False narratives, omission of important information SHIFTS IN APPROACH: Shift away from pathologization o From disease-based to identity-based model Explicit endorsement of the provision of gender affirming care to those with non-binary identities Shift towards a range of care providers (including GPs, NPs and nurses) doing assessments and delivering gender affirming care WORLD PROFESSIONAL ASSOCIATION FOR TRANSGENDER HEALTH (WPATH): Mission: to promote evidence-based care, education, research, advocacy, public policy, and respect in transsexual and transgender health “Standards of Care”: guidelines for working with children, adolescents and adults, to provide appropriate mental health, endocrine, surgical, reproductive, voice/communication, preventative and primary care o Evidence-based; represent consensus among leading international experts in trans care GENDER DYSPHORIA: Discomfort or distress that is caused by a discrepancy between a person’s gender identity and that person’s sex assigned at birth (and the associated gender role and/or primary and secondary sex characteristics) GENDER AFFIRMATION: Social Steps Name and pronoun change Clothing, makeup, hairstyle Medical Intervention Puberty blockade Hormone therapy Other individualized intervention Surgical Intervention Upper body surgeries o Male chest contouring o Breast augmentation Gonadectomy o Hysterectomy o Orchiectomy Genital Reconstruction o Vaginoplasty o Metoidioplasty o Phalloplasty Other procedures: o Electrolysis o Tracheal shave o Facial feminization MEDICATIONS FOR GENDER AFFIRMATION: Off-label use Contraindications are often relative o Carefully weigh risks and benefits of treatment vs. no treatment o Actively mitigate risks Research is limited Thorough informed consent process (i.e. forms) PATHWAY TO MEDICAL TREATMENT: Step 1 Pre-treatment readiness assessment: A range of care providers with training and experience (GP, NP, pediatrician, social workers, nurses, psychiatrists and psychologists) will complete the assessment and either write a letter of recommendation for hormone therapy or initiate treatment Step 2 Initiation of hormone therapy: Medical doctor or nurse practitioner with training & experience + physical assessment (if not already done) Step 3 Maintenance of treatment: Any medical doctor or NP (with specialist support as needed) READINESS ASSESSMENT: Does this person meet the WPATH criteria for treatment? Are they ready from a psychosocial point of view? Do they have a plan for ongoing care and support? o If not, how can we support them to ensure they get the medically necessary txt? Is further evaluation required? WPATH CRITERIA: 1. Persistent well-documented gender dysphoria 2. Capacity to make a fully informed decision and to consent for treatment 3. If significant medical/mental concerns are present, they must be reasonably well-controlled 4. Age of majority in a given country GENERAL TIPS TO KEEP IN MIND: Focus on presenting concern Do not overly focus on gender Ask relevant health questions and be prepared to justify your questions Recognize that the need to affirm gender may be prioritized over other health issues Be prepared that due to stigma & past negative experiences some patients may seem defensive REVERSIBLE MEDICAL INTERVENTION: PUBERTY BLOCKERS: LEUPROLIDE (a GnRH analogue) For younger youth, started at Tanner 2 development or later Blocks natural puberty o Gives time to mature and consider decision o Eases distress associated with pubertal changes IM injection q4-12 weeks Dosing is weight-based (typically 7.5 15 mg monthly) 5% risk of sterile abscess OPTIONS FOR SUPPRESSION OF MONTHLY BLEEDING: Medroxyprogesterone 150 mg IM q12 weeks Continuous OCP Progesterone-releasing IUD o Higher progesterone dose = more effective
Transcript
Page 1: “Standards of Care”...Enlargement of external genitals (clitoris) 3-6 months 1-2 years Internal genital (vagina) atrophy 3-6 months 1-2 years Deepened voice 3-12 months 1-2 years

Lecture 3 Gender Affirming Medical Therapy Townsend

HISTORICAL CONTEXT OF TRANSGENDER HEALTHCARE:

• Care limited to specialized gender clinics (psychiatry,

psychology, sexual medicine, endocrinology)

• Pathologization of trans identities

• Reparative therapy

• Excessive gate-keeping

• Lengthy assessments prior to treatment

• Expectation of binary transition

BARRIERS TO CARE AND CONSEQUENCES:

BARRIERS • Prior negative experiences in healthcare settings

• Fears or expectations of negative experiences

• Body dysphoria (and clinician discomfort with trans bodies)

• Lack of provider comfort, knowledge/trans competence

CONSEQUENCES • Postponing care until problems are more serious

• Avoidance of care leads to missed screening, untreated health conditions

• Self-medicating (hormone therapy)

• False narratives, omission of important information

SHIFTS IN APPROACH:

• Shift away from pathologization

o From disease-based to identity-based model

• Explicit endorsement of the provision of gender

affirming care to those with non-binary identities

• Shift towards a range of care providers (including

GPs, NPs and nurses) doing assessments and

delivering gender affirming care

WORLD PROFESSIONAL ASSOCIATION FOR TRANSGENDER HEALTH (WPATH):

• Mission: to promote evidence-based care, education, research, advocacy, public policy, and

respect in transsexual and transgender health

• “Standards of Care”: guidelines for working with children, adolescents and adults, to provide

appropriate mental health, endocrine, surgical, reproductive, voice/communication,

preventative and primary care

o Evidence-based; represent consensus among leading international experts in trans care

GENDER DYSPHORIA:

• Discomfort or distress that is caused by a

discrepancy between a person’s gender identity and

that person’s sex assigned at birth (and the

associated gender role and/or primary and

secondary sex characteristics)

GENDER AFFIRMATION:

Social Steps • Name and pronoun change

• Clothing, makeup, hairstyle

Medical Intervention

• Puberty blockade

• Hormone therapy

• Other individualized intervention

Surgical Intervention

• Upper body surgeries o Male chest contouring o Breast augmentation

• Gonadectomy o Hysterectomy o Orchiectomy

• Genital Reconstruction o Vaginoplasty o Metoidioplasty o Phalloplasty

• Other procedures: o Electrolysis o Tracheal shave o Facial feminization

MEDICATIONS FOR GENDER AFFIRMATION:

• Off-label use

• Contraindications are often relative

o Carefully weigh risks and benefits of

treatment vs. no treatment

o Actively mitigate risks

• Research is limited

• Thorough informed consent process (i.e. forms)

PATHWAY TO MEDICAL TREATMENT:

Step 1 Pre-treatment readiness assessment:

• A range of care providers with training and experience (GP, NP, pediatrician, social workers, nurses, psychiatrists and psychologists) will complete the assessment and either write a letter of recommendation for hormone therapy or initiate treatment

Step 2 Initiation of hormone therapy:

• Medical doctor or nurse practitioner with training & experience

• + physical assessment (if not already done)

Step 3 Maintenance of treatment:

• Any medical doctor or NP (with specialist support as needed)

READINESS ASSESSMENT:

• Does this person meet the WPATH criteria for treatment?

• Are they ready from a psychosocial point of view?

• Do they have a plan for ongoing care and support?

o If not, how can we support them to ensure they get the medically necessary txt?

• Is further evaluation required?

WPATH CRITERIA:

1. Persistent well-documented gender dysphoria

2. Capacity to make a fully informed decision and to consent for treatment

3. If significant medical/mental concerns are present, they must be reasonably well-controlled

4. Age of majority in a given country

GENERAL TIPS TO KEEP IN MIND:

• Focus on presenting concern

• Do not overly focus on gender

• Ask relevant health questions and be prepared to

justify your questions

• Recognize that the need to affirm gender may be

prioritized over other health issues

• Be prepared that due to stigma & past negative

experiences some patients may seem defensive

REVERSIBLE MEDICAL INTERVENTION:

PUBERTY BLOCKERS: LEUPROLIDE (a GnRH analogue)

• For younger youth, started at Tanner 2 development or later

• Blocks natural puberty

o Gives time to mature and consider decision

o Eases distress associated with pubertal changes

• IM injection q4-12 weeks

• Dosing is weight-based (typically 7.5 – 15 mg monthly)

• 5% risk of sterile abscess

OPTIONS FOR SUPPRESSION OF MONTHLY BLEEDING:

• Medroxyprogesterone 150 mg IM q12 weeks

• Continuous OCP

• Progesterone-releasing IUD

o Higher progesterone dose = more effective

Page 2: “Standards of Care”...Enlargement of external genitals (clitoris) 3-6 months 1-2 years Internal genital (vagina) atrophy 3-6 months 1-2 years Deepened voice 3-12 months 1-2 years

Lecture 3 Gender Affirming Medical Therapy Townsend

FEMINIZING THERAPY: ESTROGEN + T BLOCKERS

• GOAL: to reduce testosterone-related secondary sex characteristics, induce estrogen-related secondary sex characteristics and reduce gender dysphoria

• Start low and titrate q4-6 weeks (or more slowly if clinically indicated or desired by patient)

• Dose changes based on lab values, patient goals, response, side effects

SYSTEMIC TESTOSTERONE BLOCKERS:

• GOAL: suppress testosterone to female range (or higher if desired by pt)

• Allows us to use lower doses of estrogen than otherwise needed

• Typically discontinued post-gonadectomy

SPIRONOLACTONE:

MECHANISM K+ sparing diuretic with anti-androgen effect

CONTRAINDICATIONS Renal failure, hyperkalemia

DOSE Starting dose = 50 mg daily, and titrate to typical range of 200-300 mg daily

SIDE EFFECTS Frequent urination, dizziness, fatigue

INTERACTIONS Medications that lower BP or increase risk of hyperkalemia (ex// ACEIs, ARBs)

MONITOR Blood pressure, electrolytes, Cr

CYPROTERONE:

MECHANISM Acts via blockade of the androgen receptor, inhibition of LH

CONTRAINDICATIONS Liver disease

DOSE Starting dose = 25 mg daily, and titrate to typical range of 25-100 mg daily

SIDE EFFECTS Depression

INTERACTIONS Cyproterone is a major CYP3A4 substrate = possible interactions with statins, anti-coagulants, anti-diabetic agents

MONITOR Mood, ALT

COVERAGE Requires special authority application

ESTROGEN THERAPY:

• GOAL: to maintain testosterone levels in the female range, estrogen

levels in the 300-800 pmol/L range, minimize side effects and maintain

expected rates of physical changes (based on patient preference)

• Typically used lifelong, lower dosing maybe possible post-gonadectomy

ESTROGEN:

MECHANISM Direct action on estrogen receptors

CONTRAINDICATIONS Unstable ischemic cardiac disease, estrogen-dependent cancer, end-stage liver disease

DOSE Depending on dosage form

SIDE EFFECTS Nausea, headaches, decreased libido

INTERACTIONS Estrogen is a major substrate of CYP3A4 = possible interactions with anti-epileptics, HIV medications, St. John’s Wort

RISKS VTE, increased triglycerides, gall stones, liver inflammation

MONITOR E level, ALT, metabolic parameters

ESTROGEN DOSING:

ORAL (17B ESTRADIOL)

Starting dose = 1-2 mg and titrate to typical range of 4-8 mg daily

ESTRADIOL PATCH

Starting dose = 50 mcg and titrate to typical range of 200-300 mcg twice weekly

• Indicated if > 40 yrs + risk factors (ex// smoking)

• Requires special authority

ESTRADIOL VALERATE INJECTION

Starting dose = 5 mg IM q2 weeks and titrate to usual dose of 10-20 mg q2wks

• Only available compounded

EFFECTS & EXPECTED TIME COURSE (estrogen + blocker):

Effect Expected Onset

Expected Max Effect

Body fat re-distribution 3-6 months 2-5 years

↓ muscle mass/strength 3-6 months 1-2 years

Softening of skin / decreased oiliness

3-6 months Unknown

↓ libido 1-3 months 1-2 years

↓ spontaneous arousal (erections)

1-3 months 3-6 months

Breast growth 3-6 months 2-3 years

↓ testicular volume 3-6 months 2-3 years

Changes to body & facial hair 6-12 months > 3 years

Fertility * variable effects

RISKS (estrogen + T-blocker):

Risk level Estrogen Likely increase risk VTE, ↑ TGs, gallstones, ↑ LEs, ↑ wt

Likely increase risk with additional risk factors

Cardiovascular disease

Possible increase risk ↑ BP, ↑ prolactin, prolactinoma

Possible increase risk with additional risk factors

Type 2 diabetes

No increase risk or inconclusive Breast cancer

LAB MONITORING (estrogen + T-blocker):

• GOAL: typically to maintain hormone levels in the female range, induce

physical changes at expected rate, and minimize adverse effects

Baseline (and q6-12m thereafter):

• Testosterone

• CBC, GFR, TSH, ALT

• Electrolytes, fasting glucose, lipids

Following dose changes: • Testosterone, estrogen levels

• ALT, electrolytes

FINASTERIDE:

• May augment use of spironolactone or cyproterone

• Not typically used as main anti-androgen

MECHANISM Peripheral action only – inhibits conversion of testosterone to dihydrotestosterone

DOSE Finasteride 5 mg – ¼ tab daily or ½ tab q2 days

SIDE EFFECTS Typically none, hypotension, reduced libido uncommon

PROGESTERONE:

• GOAL: use is controversial (benefits unproven, risks may be increased);

typically for breast growth, other reasons include libido, sleep

• 3-6 month trial is reasonable for a fully informed patient

DOSE Micronized progesterone: starting dose 100 mg daily, can titrate up to 400 mg daily Medroxyprogesterone: starting dose 10 mg daily, can titrate up to 15 mg daily

SIDE EFFECTS Weight gain, mood changes, edema

INTERACTIONS Progesterone is a major substrate of CYP3A4 and CYP2C19; decreased effect of anti-coagulants, anti-diabetics

RISKS Combo of estrogen and progesterone increased risk of blood clots, heart disease, breast cancer

MONITOR E level, ALT, metabolic parameters

Page 3: “Standards of Care”...Enlargement of external genitals (clitoris) 3-6 months 1-2 years Internal genital (vagina) atrophy 3-6 months 1-2 years Deepened voice 3-12 months 1-2 years

Lecture 3 Gender Affirming Medical Therapy Townsend

FEMINIZING THERAPY:

COMMON SIDE EFFECTS AND OTHER CONCERNS:

Persistent dizziness/postural hypotension

• Caused by spironolactone, usually temporary and mild

• If severe or persistent switch to cyproterone (eligible for special authority)

Low libido • Consider maintaining testosterone at higher level

• Trial of progesterone

Difficulty having/maintaining arousal (erections)

• Consider maintaining testosterone at a higher level

• Trials of phosphodiesterase-5 inhibitor (Sildenafil, Tadalafil)

Elevated prolactin • Common and typically benign with estrogen therapy

• If > 80 mcg/L or if symptomatic (headaches, visual changes, excessive galactorrhea), consider pituitary imaging

Elevated transaminases • Usually transient unless another cause of hepatic dysfunction identified

Scalp hair loss • Minoxidil 5% and/or finasteride 2.5 mg q2days

Post-vaginoplasty vaginal discharge • The lining of the vagina is inverted penile/scrotal skin (squamous epithelium)

• Oral antibiotics usually ineffective

• Intravaginal metronidazole gel bid + plain water douching recommended

MASCULINIZING THERAPY: TESTOSTERONE

• GOALS: to reduce estrogen-related secondary sex characteristics, induce testosterone-related secondary sex characteristics & reduce gender dysphoria

• Start low and titrate q4-6 weeks

• Base dose changes on lab values, patient goals, response, side effects

TESTOSTERONE:

• GOAL: to maintain mid-injection cycle levels in the middle-high end of

male range, minimize side effects and maintain expected rates of

physical change (based on patient preferences)

• Typically used lifelong, lower dosing may be possible post-gonadectomy

• Available in several forms; special authority application required

TESTOSTERONE THERAPY:

MECHANISM Direct action on androgen receptors

CONTRAINDICATIONS Pregnancy, active androgen-sensitive cancer, unstable ischemic cardiac disease, uncontrolled psychosis or mania

DOSE Depending on dosage form

SIDE EFFECTS Acne, insomnia, libido changes

INTERACTIONS Vit K antagonists, anti-diabetics, cyclosporine

RISKS Polycythemia, dyslipidemia, sleep apnea

TESTOSTERONE DOSING:

INJECTABLE Starting dose = 25 mg IM/SC weekly and titrate to maintenance dose of 50-100 mg weekly

PATCH Starting dose = 2.5 mg daily and titrate to typical dose of 5-10 mg daily

GEL/CREAM Starting dose = 2.5 g daily and titrate to a typical dose of 5-7.5 g daily

EFFECTS AND EXPECTED TIME COURSE (testosterone):

Effect Expected Onset Expected Max Effect

Skin oiliness/acne 1-6 months 1-2 years

Facial/body hair growth 3-6 months 3-5 years

Scalp hair loss > 12 months Variable

↑ muscle mass/strength 6-12 months 2-5 years

Body fat redistribution 3-6 months 2-5 years

Cessation of menses 2-6 months N/A

Enlargement of external genitals (clitoris)

3-6 months 1-2 years

Internal genital (vagina) atrophy

3-6 months 1-2 years

Deepened voice 3-12 months 1-2 years

Fertility * variable effects

RISKS (testosterone):

Risk level Testosterone Likely increase risk Polycythemia, ↑ weight, acne,

balding, sleep apnea

Possible increase risk Hyperlipidemia, ↑ LEs

Possible increase risk with additional risk factors

CVD, ↑ BP, increased mania or psychosis, T2DM

No increase risk or inconclusive Breast, cervical, ovarian or uterine cancer, loss of bone density

LAB MONITORING (testosterone):

• GOAL: typically to maintain hormone levels in the male range, induce physical changes at expected rate, and minimize adverse effects

Baseline (and q6-12m thereafter): • Testosterone, CBC, ALT, fasting glucose & lipids, TSH

Following dose changes: • Testosterone, CBC, ALT

COMMON SIDE EFFECTS AND OTHER CONCERNS:

Acne • Typically most problematic in the first year of hormone therapy

• Treat as per usual, consider lower doses or switching to testosterone type if persistent

Scalp hair loss • Minoxidil – will not impact facial hair growth; finasteride – will inhibit facial hair growth

Polycythemia • Usually a misinterpretation – ensure the HB/HCT are being interpreted based on male laboratory ranges

• If HB > 175 g/L or HCT > 0.52, or if symptomatic (headaches, facial flushing), increase frequency of dosing to weekly, reduce dose, or switch to a patch/gel to minimize peak/trough variation

Elevated transaminases • Usually transient unless another cause of hepatic dysfunction identified

Unexpected bleeding • Bleeding typically supressed in 6m of starting testosterone; unexplained persistent abnormal bleeding should be evaluated

• Evaluate for missed/inconsistent/excessive testosterone dosing; check trough testosterone levels, estradiol, LH, FSH o Testosterone can convert to estrogen with theoretical risk of endometrial proliferation

• Consider more frequent dosing (weekly), or dose adjustment

Internal genital (vaginal) dryness

• Topical estrogen inside the genital opening (vagina)

• Estradiol cream 0.5 – 1 g twice weekly or estradiol tablet 10 mcg twice weekly

Page 4: “Standards of Care”...Enlargement of external genitals (clitoris) 3-6 months 1-2 years Internal genital (vagina) atrophy 3-6 months 1-2 years Deepened voice 3-12 months 1-2 years

Lecture 3 Gender Affirming Medical Therapy Townsend

HORMONE THERAPY FOLLOW-UP:

• Follow-up q4-6 weeks while titrating, and then q6-12 months

• Review effects of hormones, dose, side effects, mood, supports, social challenges

• Check BP, other physical exam as indicated

• Review labs

• Adjust dose if indicated

HORMONE THERAPY VARIATIONS:

• As always, care should be individualized

• Some possible variations:

o Lower dose of hormones

o More gradual titration

o Temporary use of hormones

o Using T-blocker w/o estrogen (not recommended long-term)


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