Precocious puberty

Last updated: November 14, 2025

Summary

Precocious puberty is the appearance of secondary sexual characteristics before 8 years of age in girls and 9 years of age in boys. Precocious puberty is classified as central precocious puberty, resulting from early gonadotropin-releasing hormone (GnRH) secretion causing activation of the hypothalamic-pituitary-gonadal axis, or peripheral precocious puberty, resulting from sex hormone production that is not driven by GnRH secretion. Central precocious puberty may be idiopathic or caused by CNS pathology or genetic syndromes. Causes of peripheral precocious puberty include increased sex hormone production from adrenal or gonadal tumors, functional ovarian cysts, exogenous steroid use, and hypothyroidism. Clinical evaluation involves a focused history and physical examination, including a pediatric growth assessment and sexual maturity rating, to distinguish precocious puberty from benign pubertal variants. Initial diagnostic evaluation includes laboratory testing (gonadotropin and sex hormone levels) and a bone age assessment. Targeted testing to determine the underlying cause is based on clinical presentation and initial results. Management is based on the underlying cause. GnRH analogs may be considered in some patients with central precocious puberty.

Classification

By location ^[1]^[2]

Central precocious puberty

Caused by early onset of GnRH secretion
Early activation of the hypothalamic-pituitary-gonadal axis → abnormally early initiation of pubertal changes → early development of secondary sexual characteristics
♀ > ♂ (10:1) ^[1]
The sequence and rate of progression of pubertal development are symmetrical and align with those in normal puberty, but puberty occurs at an early age. ^[1]^[3]

Peripheral precocious puberty

Early development of secondary sexual characteristics caused by an increase in sex hormones that is not driven by GnRH secretion
The sequence and rate of progression of pubertal development may be incomplete, asymmetrical, or discordant from those in normal puberty. ^[1]^[3]

By phenotype ^[4]

Isosexual precocious puberty

Early development of secondary sexual characteristics that match the individual's biological sex
Can occur in central and peripheral precocious puberty

Heterosexual precocious puberty

Early development of secondary sexual characteristics that are discordant with the individual's biological sex
Can occur in peripheral precocious puberty (e.g., McCune-Albright syndrome, Leydig cell tumors, congenital adrenal hyperplasia)

Etiology

Etiology of central precocious puberty ^[1]^[4]^[5]

Idiopathic (most common cause in girls)
CNS lesions
- Intracranial tumors (e.g., hypothalamic hamartoma, optic pathway glioma)
- Hydrocephalus
- Brain injury (e.g., traumatic brain injury, radiation injury)
- Intracranial infections (e.g., encephalitis, meningitis)
Genetic syndromes: neurofibromatosis type 1, tuberous sclerosis

Boys are more likely than girls to have an identifiable cause of central precocious puberty (e.g., CNS lesions). ^[1]^[4]

Hypothalamic hamartoma is the most common CNS lesion in central precocious puberty. ^[4]

Etiology of peripheral precocious puberty ^[1]^[2]^[4]

Increased androgen production
- Congenital adrenal hyperplasia
- Adrenocortical tumors
- Androgen-producing gonadal tumors (e.g., Sertoli-Leydig cell tumor, Leydig cell tumor)
Increased estrogen production
- McCune-Albright syndrome
- Functional ovarian cyst
Tumors that produce β-hCG ^[4]^[6]
- Embryonal carcinoma
- Testicular choriocarcinoma
Primary hypothyroidism
Exposure to exogenous steroids (e.g., OCPs, estrogen-containing creams, testosterone gel)

Central precocious puberty has a central cause (e.g., hypothalamic lesions) and high GnRH levels, while peripheral precocious puberty has a peripheral cause (e.g., germ cell tumors) without elevated GnRH levels.

Obesity is associated with early pubertal development. See "Factors affecting timing and progression of puberty." ^[7]^[8]

Clinical evaluation

The clinical presentation depends on the underlying condition.

Focused history ^[1]^[2]

Pubertal development
- Age of onset of secondary sexual characteristic development, e.g.:
  - Pubic and axillary hair
  - Body odor
  - Breast development
  - Testicular development
- Sequence and pattern of development
- Symmetry in development of breasts and testes
- Complete vs. incomplete development (e.g., isolated premature thelarche, adrenarche, or menarche)
- Additional signs of puberty (e.g., voice change, acne, vaginal bleeding)
Associated features of an underlying cause
- Neurological symptoms (e.g., headache, vision changes)
- Symptoms of hypothyroidism or clinical features of thyrotoxicosis
- Abdominal pain
Personal medical history
- History of brain tumor or head trauma
- Cancer treatments (e.g., chemotherapy, radiation)
- Sex steroid use (e.g., OCPs, topical estrogen or testosterone)
Family history: timing of parental puberty ^[2]
Environmental exposures: endocrine-disrupting chemicals (e.g., lavender oil, phthalates)

Focused examination ^[1]^[2]

Pediatric growth assessment
- Standard pediatric growth parameters (e.g., height, weight, and BMI)
- Growth velocity
Evaluation for physical changes during puberty
- Sexual maturity rating ^[1]
- Facial and axillary hair
- Acne
Evaluation for underlying cause
- Abdominal and testicular examination: for gonadal tumors
- Vaginal examination to assess for signs of:
  - Estrogen exposure (e.g., dull pink vaginal mucosa, vaginal discharge)
  - Virilization (e.g., clitoromegaly)
- Skin examination: for café au lait macules (seen in McCune-Albright syndrome, neurofibromatosis)
- Thyroid examination
- Neurological examination: for suspected CNS pathology

Children with precocious puberty may have accelerated growth in adolescence but typically have shorter than average stature in adulthood due to early closure of the epiphyseal plates. ^[1]

Diagnostics

Approach

Suspected benign pubertal variant : Consider observation for 3–6 months before diagnostic testing.
Multiple and/or progressive development of secondary sexual characteristics: Obtain initial studies, including gonadotropins and bone age radiography.
- LH > 0.3 IU/L: targeted testing for etiology of central precocious puberty ^[2]
- LH < 0.3 IU/L with suspected central precocious puberty: GnRH stimulation test
- Prepubertal LH levels
  - Suspected peripheral precocious puberty: targeted testing for etiology of peripheral precocious puberty
  - Suspected benign pubertal variant: observation
Diagnostic uncertainty: Refer to endocrinology for further evaluation.

Patients with normal initial laboratory studies and isolated examination findings suggesting benign pubertal variants can be observed for 3–6 months before further workup. ^[1]

The diagnostic approach to precocious puberty in children with obesity is the same as in children with normal body weight. ^[8]

Initial diagnostic studies ^[1]

Laboratory studies

LH and FSH
- Typically increased in central precocious puberty
- Prepubertal levels suggest peripheral precocious puberty or a benign pubertal variant.
Testosterone (boys) or estradiol (girls)
- Typically increased in both central and peripheral precocious puberty
- Estradiol > 100 pg/ml suggests an ovarian source (e.g., ovarian tumor). ^[1]

Obtaining laboratory studies in the early morning is preferred. ^[9]

Bone age radiography

Most commonly performed as x-ray of nondominant hand and wrist
Advanced bone age (> 2 standard deviations) compared to chronological age suggests central or peripheral precocious puberty rather than benign pubertal variant

Advanced bone age is common in children with obesity, which limits the utility of bone age radiography in distinguishing between precocious puberty and benign pubertal variants.^[8]

Additional diagnostic studies ^[1]

Obtain additional testing based on clinical presentation and initial diagnostics. Consult a specialist (e.g., endocrinology) as needed.

Suspected central precocious puberty despite LH < 0.3 IU/L ^[1]^[2]

GnRH stimulation test
- LH elevation after GnRH stimulation: central precocious puberty
- No LH elevation after GnRH stimulation: peripheral precocious puberty or benign pubertal variant
Pelvic imaging: Consider in girls to assess uterine and ovarian volume in the case of diagnostic uncertainty.

Targeted testing for underlying cause

Central precocious puberty and/or suspected CNS pathology: MRI brain ^[2]^[9]
Signs of hypothyroidism or signs of hyperthyroidism: TSH
Signs of hyperandrogenism: serum DHEA-S, 17-hydroxyprogesterone
Suspected gonadal tumor
- Ultrasound pelvis or testicles
- β-hCG in boys with suspected germ cell tumors
Suspected adrenal tumor: adrenal imaging

CNS imaging is recommended in all boys and in girls < 6 years of age with central precocious puberty. Use shared decision-making to determine the need for imaging in girls 6–8 years of age. ^[2]^[9]

Common causes

Common causes of precocious puberty ^[1]^[2]^[4]
		Characteristic clinical features	Diagnostic findings	Management
Central precocious puberty	Idiopathic	Early puberty with normal sequence	Pubertal levels of LH and FSH (LH > 0.3 IU/L) Pubertal levels of testosterone or estradiol ^[5] GnRH stimulation test: ↑ LH Advanced bone age Ultrasound: ↑ gonad volume	GnRH agonists in selected cases
Central precocious puberty	CNS abnormalities	Early puberty with normal sequence Neurological findings (e.g., seizure, vision changes)	Pubertal levels of LH and FSH (LH > 0.3 IU/L) MRI brain: may be abnormal depending on cause	GnRH agonists in selected cases Treat the underlying cause.
Peripheral precocious puberty	Gonadal mass	Testicular or adnexal mass on examination Signs of hyperestrogenism and/or vaginal bleeding in girls ^[4]	↑ Testosterone or estradiol ↓ LH and FSH Ultrasound: gonadal mass	See “Management of adnexal mass.” See “Management of testicular tumors.”
	Congenital adrenal hyperplasia ^[10]	Signs of hyperandrogenism Premature pubarche	↑ 17-hydroxyprogesterone Positive ACTH stimulation test	Refer to pediatric endocrinology. Glucocorticoid therapy
	Adrenal tumor	Signs of hyperandrogenism Premature pubarche	↑ Testosterone or estradiol ↓ LH and FSH ↑ DHEA-S Adrenal mass on imaging	Surgical resection
	McCune-Albright syndrome ^[11]	Café au lait macules Scoliosis Intermittent vaginal bleeding	↑ Testosterone or estradiol ↓ LH and FSH Bone imaging : fibrous dysplasia Ultrasound: ovarian cysts; testicular abnormalities	Refer to pediatric endocrinology and genetics.
	Exposure to exogenous hormones	Normal puberty occurring early	↑ Testosterone or estradiol ↓ LH and FSH	Discontinue causative agent(s).
	Hypothyroidism	Premature thelarche Premature testicular development	↑ TSH ↓ LH and FSH	Levothyroxine replacement

Management

Manage precocious puberty in consultation with a pediatric specialist as appropriate (e.g., endocrinology, neurology, surgery). ^[1]^[2]

Management of central precocious puberty ^[1]^[2]^[12]

GnRH agonists (e.g., leuprolide, buserelin, goserelin, histrelin) ^[2]^[9]
- Indications
  - Preservation of height potential ^[2]
  - Promotion of psychosocial well-being
  - Prevention of early menarche and sexual maturity ^[2]
- Duration of therapy: based on patient's height potential and ability to tolerate puberty
Expectant management may be considered in the absence of indications for GnRH agonists.
Management of CNS lesions, if present
Management of associated psychological stress (e.g., anxiety) as necessary

Childhood obesity is not a contraindication to GnRH agonists in children with precocious puberty. ^[8]

Management of peripheral precocious puberty ^[1]

Treat the underlying cause, e.g.:

Hormone-producing tumor: surgery ^[4]
Congenital adrenal hyperplasia: cortisol replacement (see “Treatment of congenital adrenal hyperplasia”)
Ovarian cysts
- Spontaneous resolution is common.
- Surgery may be indicated for complications.
- See “Management of ovarian cysts” for details.

Mimics

Benign variants of puberty ^[2]^[13]

Benign pubertal variants involve isolated development of secondary sexual characteristics and prepubertal pattern of linear growth.
Observation over 4–6 months is usually appropriate. ^[2] ^[1]^[13]
Children with progressive pubertal development and/or rapid linear growth during this period should be evaluated for precocious puberty.

Benign variants of puberty ^[2]
	Description	Clinical features	Diagnostic findings
Premature adrenarche ^[14]^[15]	Premature maturation of the adrenal zona reticularis (adrenarche) leading to early ↑ in androgen secretion Associated with obesity, insulin resistance Most common cause of premature pubarche ♀ > ♂	Premature pubarche: growth of pubic hair in girls aged < 8 years and boys aged < 9 years Axillary hair Body odor Seborrhea, acne No enlargement of penis, clitoris, or breasts. Growth velocity: typically normal ^[1]	↑ DHEA-S for age Normal gonadotropins, estradiol, and testosterone levels Bone age: normal or slightly advanced ^[14]
Idiopathic premature pubarche ^[14]	Premature onset of pubarche without evidence of increased androgens	Isolated premature pubarche	Normal DHEA-S for age Normal bone age
Premature thelarche	Isolated nonprogressive breast tissue development in girls < 8 years of age (often < 2 years of age) ^[2]	Palpable glandular breast tissue ^[1] Other secondary sexual characteristics are absent.	Clinical diagnosis Diagnostics for precocious puberty indicated if breast size increases over 4–6 months ^[2]
Premature menarche	Isolated prepubertal vaginal bleeding	Uterine bleeding: ≤ 6 episodes ^[2] Absence of other secondary sexual characteristics	Exclusion of other causes of vaginal bleeding in children, e.g.: Trauma Infection Sexual abuse

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