Delayed puberty medical therapy: Difference between revisions

	Delayed puberty Microchapters
Home
Patient Information
Overview
Historical Perspective
Classification
Pathophysiology
Causes
Differentiating Delayed puberty from other Diseases
Epidemiology and Demographics
Risk Factors
Screening
Natural History, Complications and Prognosis
Diagnosis
Diagnostic Criteria
History and Symptoms
Physical Examination
Laboratory Findings
Electrocardiogram
X Ray
CT
MRI
Ultrasound
Other Imaging Findings
Other Diagnostic Studies
Treatment
Medical Therapy
Surgery
Primary Prevention
Secondary Prevention
Cost-Effectiveness of Therapy
Future or Investigational Therapies
Case Studies
Case #1
Delayed puberty medical therapy On the Web
Most recent articles
Most cited articles
Review articles
CME Programs
Powerpoint slides
Images
American Roentgen Ray Society Images of Delayed puberty medical therapy All Images X-rays Echo & Ultrasound CT Images MRI
Ongoing Trials at Clinical Trials.gov
US National Guidelines Clearinghouse
NICE Guidance
FDA on Delayed puberty medical therapy
CDC on Delayed puberty medical therapy
Delayed puberty medical therapy in the news
Blogs on Delayed puberty medical therapy
Directions to Hospitals Treating Delayed puberty
Risk calculators and risk factors for Delayed puberty medical therapy

← Older edit Newer edit →

VisualWikitext

Revision as of 17:16, 13 September 2017

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief:

Overview

Medical Therapy

General approach to pharmacological medical therapy for delayed puberty^[1]

Delayed Puberty

Initial assessment

• Clinical history
• Physical examinations
• Pubertal phenotype
• Left wrist radiograph for bone age

Unremarkable

Abnormal

Chronic disease

• Delayed puberty
• Lack of growth spurt
• Bone age delayed upon chronological age

• Possibility of chromosomal disorder
• Bone age may delayed

• Chronic disease
• Decreased growth rate or short stature
• Bone age delayed upon chronological age

Diagnosis:
• Constitutional delay of growth and puberty (CDGP)
• Gonadotropin deficiency
• Primary gonadal failure
• Extreme athletic exercise

Diagnosis:
Girls:
• Turner syndrome
Boys:
• Klinefelter syndrome

Diagnosis:
• Hypopituitarism
• Chronic systemic diseases
• Anorexia nervosa
• Malnutrition
• Kallman syndrome
• Iatrogenic

Actions:
• Evaluation hypothalamus-pituitary-gonadal axis
• Consider an MRI to exclude the CNS lesions

Actions:
• Chromosome analysis (Karyotyping)

Actions:
• Upon the underlying disease

Treatment:
1. Psychologic support
2. Observation
3. Sex hormone replacement therapy

Treatment:
1. Psychologic support
2. Sex hormone replacement
3. Excision of ovaries in Turner syndrome because of risk of malignancy

Generally, the main pharmacological medical therapy for delayed puberty is sex hormone replacement therapy.
The aim of treatment is to initiate the puberty progress and to merge the secondary sexual characteristics in patients.
Regarding that the delayed puberty involve only adolescents, all of the therapy options are for them.

Delayed puberty^[2]

1 Stage 1 - Constitutional delay of growth and puberty
- 1.1 Boys
  - Preferred regimen (1): Testosterone, not indicated before 14 years of age
    - Initial dose: 50-100 mg IM every 4 weeks for 3-6 months
    - Repeated treatment: To add 25-50 mg in dose (maximum, 100 mg per dose)
  - Preferred regimen (2): Letrozole 2.5 mg PO per day
  - Preferred regimen (3): Anastozole 1mg PO per day
- 1.2 Girls
  - Preferred regimen (1): Ethinyl estradiol (EE)
    - Initial dose: 2 μg PO per day for 6-12 months
    - Repeated treatment: Increase to 5 μg PO per day after 6-12 months
  - Preferred regimen (2): 17β-estradiol (pill)
    - Initial dose: 5 μg/kg PO per day for 6-12 months
    - Repeated treatment: Increase to 10 μg/kg PO per day after 6-12 months
  - Preferred regimen (3): 17β-estradiol (transdermal patch)
    - Initial dose: 3.1-6.2 μg (1/8-1/4 of 25 μg patch) per day for 6 months
    - Repeated treatment: Increase 3.1-6.2 μg (1/8-1/4 of 25 μg patch) per day every 6 months
  - Preferred regimen (4): Conjugated equine estrogens (CEE)
    - Initial dose: 0.1625 mg PO per day for 6-12 months
    - Repeated treatment: Titrating to 0.325 mg PO per day after 6-12 months
  - Alternative regimen (1): Progestogens/Progestins in various formulations, only if treatment last more than 12 months

2 Stage 2 - Hypogonadism
- 2.1 Pediatric
  - 2.1.1 Boys
    - Preferred regimen (1): Testosterone, can be started after 12 years of age
      - Initial dose of 50 mg IM per month
      - Increase with 50 mg in dose IM every 6-12 months
      - After reaching 100-150 mg IM monthly, decrease interval to every 2 weeks
    - Preferred regimen (2): Pulsatile GnRH
      - Initial dose: 5-25 ng/kg/pulse SC every 90-120 min
      - Continued treatment: Increase to 25-600 ng/kg/pulse SC every 90-120 min
    - Alternative regimen (1): Testosterone undecanoate 1000 mg IM every 10-14 weeks
    - Alternative regimen (2): Testosterone gel, apply at bed time
      - Started when approximately 50% adult dose has been achieved with intramuscular testosterone
    - Alternative regimen (3): hCG plus recombinant FSH
      - hCG: 500 to 3000 IU SC or IM twice weekly, increased to every 2 days
      - rhFSH: 75 to 225 IU SC 2-3 times weekly
  - 2.1.2 Girls
    - Preferred regimen (1): Ethinyl estradiol (EE)
      - Initial dose: 2 μg PO per day for 6-12 months
      - Repeated treatment: Increase every 6-12 months to 5 μg, 10 μg, and 20 μg PO per day
    - Preferred regimen (2): 17β-estradiol (pill)
      - Initial dose: 5 μg/kg PO per day for 6-12 months
      - Repeated treatment: Increase to 10 μg/kg PO per day after 6-12 months, then to 15 μg/kg, and to 20μg/kg per day
    - Preferred regimen (3): 17β-estradiol (transdermal patch)
      - Initial dose: 3.1-6.2 μg (1/8-1/4 of 25 μg patch) per day for 6 months
      - Repeated treatment: Increase 3.1-6.2 μg (1/8-1/4 of 25 μg patch) per day every 6 months
    - Preferred regimen (4): Conjugated equine estrogens (CEE)
      - Initial dose: 0.1625 mg PO per day for 6-12 months
      - Repeated treatment: Increase every 6-12 months to 0.325, 0.45, and 0.625 mg PO per day
    - Alternative regimen (1): Progestogens/Progestins in various formulations, only if treatment last more than 12 months
- 2.1 Adults
  - 2.1.1 Male
    - Preferred regimen (1): Testosterone 200 mg IM every 2 weeks
    - Preferred regimen (2): Testosterone undecanoate 1000 mg IM every 10-14 weeks
    - Preferred regimen (3): Testosterone gel 50-80 mg transdermal per day
    - Alternative regimen (1): Pulsatile GnRH
      - Initial dose: 5-25 ng/kg/pulse SC every 90-120 min
      - Continued treatment: Increase to 25-600 ng/kg/pulse SC every 90-120 min
    - Alternative regimen (2): hCG plus recombinant FSH
      - hCG: 500 to 3000 IU SC or IM twice weekly, increased to every 2 days
      - rhFSH: 75 to 225 IU SC 2-3 times weekly
  - 2.1.2 Female
    - Preferred regimen (1): Ethinyl estradiol (EE) 20 μg PO per day
    - Preferred regimen (2): 17β-estradiol (pill) 1-2 mg PO per day
    - Preferred regimen (3): 17β-estradiol (transdermal patch) 50-100 μg transdermal per day
    - Preferred regimen (4): Conjugated equine estrogens (CEE) 0.625 mg PO per day
    - Alternative regimen (1): Progestogens/Progestins 5-10 mg of medroxyprogesterone acetate (MPA) PO per day during the last 7 days of menstrual cycle
    - Alternative regimen (2): Micronized progesterone 100-200 μg PO per day

All medical therapy options for delayed puberty at a glance^[3]

	Group	Medicine	Route	Constitutional Delay of Growth and Puberty (CDGP)	Hypogonadism	Side effects	Notes
Girls	Estrogen	Ethinyl estradiol (EE)	PO	Initial dose 2 μg daily. Increase after 6-12 months to 5 μg daily	Initial dose 2 μg daily. Increase every 6 to 12 months to 5 μg, 10 μg, and 20 μg daily (adult dose).	Hepatotoxicity Increasing plasma binding proteins Higher risks of thromboembolism and arterial hypertension than natural estrogens.	Component of oral contraceptive pills. Lower dose EE oral pills are available in Europe.
		17β-estradiol	PO	Initial dose 5 μg/kg daily Increase after 6-12 months to 10 μg/kg daily	Initial dose 5 μg/kg daily Increase every 6-12 months to 10 μg/kg daily, then to 15 μg/kg, and to 20μg/kg daily. Adult dose 1-2 mg daily.	Transdermal is better than oral administration.	Natural estrogen is preferable to synthetic estrogens.
		17β-estradiol	Transdermal patch or gel	Initial dose 3.1-6.2 μg/24h (1/8-1/4 of 25 μg/24h patch) Increase by 3.1-6.2 μg/24h every 6 months	Initial dose 3.1-6.2 μg/24h (1/8-1/4 of 25 μg/24h patch) Increase by 3.1-6.2 μg/24h every 6 months. Adult dose 50-100 μg/24h	-	Patches applied overnight Topical gel applied during the day No dosage equivalent data between patches and gel available in younger patients
		Conjugated equine estrogens (CEE)	PO	Initial dose 0.1625 mg daily for 6-12 months, and then titrating to 0.325 mg daily Dosing depends on formulation	Initial dose 0.1625 mg for 6-12 months, increase every 6-12 months to 0.325, 0.45, and 0.625 mg daily Common adult dose 0.625 mg	Use cautiously because of reported increased cardiovascular risks in postmenopausal women	CEE are not estradiol precursors.
	Progestogens	Progestogens/Progestins	PO	Only if treatment continues longer than 12 months	5-10 mg of medroxyprogesterone acetate (MPA) daily during the last 7 days of menstrual cycle. Alternative: micronized progesterone, dose 100-200 μg daily.	Mild nausea Diarrhea Bloating Dizziness Hot flashes Headache	Progesterone added to induce endometrial cycling after 12-18 months of estrogen therapy: Later if estrogen dose increased slowly Sooner if break-through bleeding
	Pulsatile GnRH	Subcutaneous pump	SC	Not recommended routinely	Used for fertility	-	Very expert route of treatment Most physiological form therapy
Boys	Testosterone	Testosterone enanthate (most potent) Testosterone cypionate Testosterone propionate	IM	Not recommend for less than 14 years old. Initial dose 50-100 mg every 4 weeks for 3 to 6 months Repeated treatment with 25-50 mg increment in dose (not exceeding 100 mg)	Can administered after 12 years old. Initial dose 50 mg every 4 weeks. Increase with 50 mg increments every 6 to 12 months. After reaching 100-150 mg monthly, decrease interval to every 2 weeks. Adult dose 200 mg every 2 weeks.	Local side effects (pain, erythema, inflammatory reaction, and sterile abscess). Priapism can occur in patients with sickle cell disease.	General side effects: Erythrocytosis Weight gain Prostate hyperplasia High doses can cause premature epiphyseal closure Not for use in boys with bone age < 10 years
		Testosterone undecanoate	IM	No data available	Adult dose is 1000 mg every 10-14 weeks
		Testosterone gel	Transdermal	No data available	Initiated when approximately 50% adult dose achieved with IM testosterone Adult dose 50-80 mg daily	Local irritation Avoid close skin contact after applying
	Aromatase inhibitors	Letrozole	PO	2.5 mg daily	No data available	Decreased level of high-density lipoprotein (HDL) cholesterol Erythrocytosis Vertebral deformities^[4]	Not yet approved for this indication. After onset of puberty, may increase gonadotropin secretion and circulating testosterone levels.^[5]
	Aromatase inhibitors	Anastozole	PO	1.0 mg daily	No data available	-
	Pulsatile GnRH	Subcutaneous pump	SC	Not recommended routinely	Initial dose 5-25 ng/kg/pulse every 90-120 min Maintenance dose increase to 25-600 ng/kg/pulse	-	Very expert route of treatment Most physiological form therapy
	Combination therapy	hCG plus recombinant FSH	subcutaneous or intramuscular hCG subcutaneous rhFSH	Not recommended routinely	hCG 500 to 3000IU twice weekly Increased to every 2 days Dose adjusted based on serum testosterone levels rhFSH 75 to 225 IU 2-3 times weekly.	hCG Testicular local inflammation Maybe germ cell apoptosis	In hypogonadotropic hypogonadism with prepubertal onset, in order to testicular development and also spermatogenesis, FSH is needed. No data on effects on future fertility.
	Synthetic anabolic steroid	Oxandrolone	PO	Initial dose 0.1 mg/kg/day Maintenance 2.5 mg/day for 3–12 months	No data available	Gynecomastia Impotence Priapism Bladder irritability	Adjuvant therapy to speed up the height growth The effect would be continued after treatment
	Androgen sex steroid	Dihydrotestosterone (DHT)	IM	50 mg every 2 weeks, for 4 months	No data available	Dry skin Changes in bowel habits Dry mouth Muscle pain Increased thirst Hypertension Loss of appetite Weight loss	It can result in: Appearance of secondary sex characteristics Decreased body fat percentage with no change in IGF-I, GH, and estradiol concentrations

Other types of treatments

Low-dose oxandrolone

Reference

↑ Blondell RD, Foster MB, Dave KC (1999). "Disorders of puberty". Am Fam Physician. 60 (1): 209–18, 223–4. PMID 10414639.
↑ Palmert, Mark R.; Dunkel, Leo (2012). "Delayed Puberty". New England Journal of Medicine. 366 (5): 443–453. doi:10.1056/NEJMcp1109290. ISSN 0028-4793.
↑ Palmert, Mark R.; Dunkel, Leo (2012). "Delayed Puberty". New England Journal of Medicine. 366 (5): 443–453. doi:10.1056/NEJMcp1109290. ISSN 0028-4793.
↑ Hero M, Toiviainen-Salo S, Wickman S, Mäkitie O, Dunkel L (2010). "Vertebral morphology in aromatase inhibitor-treated males with idiopathic short stature or constitutional delay of puberty". J. Bone Miner. Res. 25 (7): 1536–43. doi:10.1002/jbmr.56. PMID 20200972.
↑ Wickman S, Dunkel L (2001). "Inhibition of P450 aromatase enhances gonadotropin secretion in early and midpubertal boys: evidence for a pituitary site of action of endogenous E". J. Clin. Endocrinol. Metab. 86 (10): 4887–94. doi:10.1210/jcem.86.10.7927. PMID 11600558.

Template:WS Template:WH

[pmid10414639-1] Blondell RD, Foster MB, Dave KC (1999). "Disorders of puberty". Am Fam Physician. 60 (1): 209–18, 223–4. PMID 10414639.

[PalmertDunkel2012-2] Palmert, Mark R.; Dunkel, Leo (2012). "Delayed Puberty". New England Journal of Medicine. 366 (5): 443–453. doi:10.1056/NEJMcp1109290. ISSN 0028-4793.

[PalmertDunkel20122-3] Palmert, Mark R.; Dunkel, Leo (2012). "Delayed Puberty". New England Journal of Medicine. 366 (5): 443–453. doi:10.1056/NEJMcp1109290. ISSN 0028-4793.

[pmid20200972-4] Hero M, Toiviainen-Salo S, Wickman S, Mäkitie O, Dunkel L (2010). "Vertebral morphology in aromatase inhibitor-treated males with idiopathic short stature or constitutional delay of puberty". J. Bone Miner. Res. 25 (7): 1536–43. doi:10.1002/jbmr.56. PMID 20200972.

[pmid11600558-5] Wickman S, Dunkel L (2001). "Inhibition of P450 aromatase enhances gonadotropin secretion in early and midpubertal boys: evidence for a pituitary site of action of endogenous E". J. Clin. Endocrinol. Metab. 86 (10): 4887–94. doi:10.1210/jcem.86.10.7927. PMID 11600558.

[1]

[2]

[3]

[4]

[5]

@@ Line 101: / Line 101: @@
 ****Alternative regimen (1): [[Progestogens]]/[[Progestins]] 5-10 mg of [[Medroxyprogesterone acetate|medroxyprogesterone acetate (MPA)]] PO per day during the last 7 days of menstrual cycle
 ****Alternative regimen (2): Micronized [[progesterone]] 100-200 μg PO per day
+=== All medical therapy options for delayed puberty at a glance<ref name="PalmertDunkel20122">{{cite journal|last1=Palmert|first1=Mark R.|last2=Dunkel|first2=Leo|title=Delayed Puberty|journal=New England Journal of Medicine|volume=366|issue=5|year=2012|pages=443–453|issn=0028-4793|doi=10.1056/NEJMcp1109290}}</ref> ===
 {| class="wikitable"
 !
@@ Line 179: / Line 181: @@
 * 5-10 mg of [[Medroxyprogesterone acetate|medroxyprogesterone acetate (MPA)]] daily during the last 7 days of [[menstrual cycle]].
 * Alternative: micronized [[progesterone]], dose 100-200 μg daily.
-|<nowiki>-</nowiki>
+|
+* Mild [[nausea]]
+* [[Diarrhea]]
+* [[Bloating]]
+* [[Dizziness]]
+* [[Hot flashes]]
+* [[Headache]]
 |Progesterone added to induce endometrial cycling after 12-18 months of estrogen therapy:
 * Later if estrogen dose increased slowly
@@ Line 190: / Line 198: @@
 |
 * Not recommended routinely
-|Used for fertility
+|
+* Used for [[fertility]]
 | -
 |
@@ Line 196: / Line 205: @@
 * Most [[physiological]] form therapy
 |-
-| rowspan="7" |'''Boys'''
+| rowspan="9" |'''Boys'''
 | rowspan="3" |[[Testosterone]]
 |
@@ Line 305: / Line 314: @@
 * In [[hypogonadotropic hypogonadism]] with prepubertal onset, in order to [[testicular]] development and also [[spermatogenesis]], [[FSH]] is needed.
 * No data on effects on future [[fertility]].
+|-
+|Synthetic [[anabolic steroid]]
+|
+* [[Oxandrolone]]
+|PO
+|
+* Initial dose 0.1 mg/kg/day
+* Maintenance 2.5 mg/day for 3–12 months
+|
+* No data available
+|
+* [[Gynecomastia]]
+* [[Impotence]]
+* [[Priapism]]
+* [[Bladder]] irritability
+|
+* [[Adjuvant therapy]] to speed up the height growth
+* The effect would be continued after treatment
+|-
+|[[Androgen]] [[sex steroid]]
+|
+* [[Dihydrotestosterone]] (DHT)
+|IM
+|
+* 50 mg every 2 weeks, for 4 months
+|
+* No data available
+|
+* [[Dry skin]]
+* [[Changes in bowel habits]]
+* [[Dry mouth]]
+* [[Muscle pain]]
+* Increased [[thirst]]
+* [[Hypertension]]
+* [[Loss of appetite]]
+* [[Weight loss]]
+|
+* It can result in:
+** Appearance of [[secondary sex characteristics]]
+** Decreased [[body fat]] percentage with no change in [[IGF-I]], [[GH]], and [[estradiol]] concentrations
 |}
+=== Other types of treatments ===
+==== Low-dose oxandrolone ====
 ==Reference==

Delayed puberty medical therapy: Difference between revisions

Revision as of 17:16, 13 September 2017

Overview

Medical Therapy

General approach to pharmacological medical therapy for delayed puberty[1]

Delayed puberty[2]

All medical therapy options for delayed puberty at a glance[3]