McCune-Albright syndrome

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	McCune-Albright syndrome;
ICD-10	Q78.1
ICD-9	756.54
OMIM	174800
DiseasesDB	7880
MedlinePlus	001217
eMedicine	ped/1386
MeSH	D005359

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

Overview

McCune-Albright syndrome is a rare genetic disorder caused by an activating mutation of the GNAS gene resulting in various phenotypic presentations. McCune-Albright syndrome typically presents with the triad of fibrous dysplasia, precocious puberty and café au lait spots in both genders. Other manifestations include hyperthyroidism, acromegaly and Cushing’s syndrome.

Historical Perspective

McCune-Albright syndrome was first discovered by physicians Donovan McCune and Fuller Albright in 1937.

Classification

Pathophysiology

The pathogenesis of McCune-Albright syndrome is characterized by increased cAMP signaling in bone, skin and endocrine tissues. In bone osteoblasts differentiation results in fibrous dysplasia. In the skin there is stimulation of melanin production resulting in café au lait macules with irregular borders. In endocrine tissues increased cAMP results in increased production of hormones depending on which tissue is affected including the gonads, thyroid, parathyroid, pituitary and adrenal glands.
The GNAS gene mutation has been associated with the development of McCune-Albright syndrome, involving the cAMP pathway-associated G-protein, Gsα. The various tissues involved in the syndrome is a result of the ubiquitous signaling of Gsα.

Causes

McCune-Albright syndrome is caused by a missense mutation of the GNAS gene alpha subunit which becomes constitutively activated. This increases intracellular cAMP which activates downstream hormones resulting in multiple tissue types being affected and mosaicism presented in its patients. ^[1]

Differentiating McCune-Albright syndrome from other Diseases

For further information about the differential diagnosis, click here

Epidemiology and Demographics

The prevalence of McCune-Albright syndrome is between 1:100,000 and 1:1,000,000 making it very rare.

Age

McCune-Albright syndrome is more commonly observed among infants and young children.

Gender

McCune-Albright syndrome affects boys and girls equally. ^[2]

Race

There is no racial predilection for McCune-Albright syndrome.

Risk Factors

There are no risk factors for McCune-Albright syndrome.

Natural History, Complications and Prognosis

Early clinical features include café-au-lait macules often shortly after or at birth.
If left untreated patients may progress to develop decreased adult stature as a result of precocious puberty. ^[1]
Common complications of McCune-Albright syndrome include rickets because of phosphate wasting and pain and fractures at fibrous dysplasia sites. ^[1]

Diagnosis

Diagnostic Criteria

The diagnosis of McCune-Albright syndrome is a clinical diagnosis. ^[1]
Though there are genetic tests available for the GNAS gene mutation with new PCR techniques for those who show clinical signs of the syndrome.
Patients who present with monostotic fibrous dysplasia are required to have evidence of the pathogenic GNAS gene my molecular testing ^[2]

Symptoms

Café au lait spot in McCune Albright syndrome with coast of Maine irregular borders

Symptoms of McCune-Albright syndrome include the following:
- Precocious puberty
  - In girls presenting with ovarian cysts with vaginal bleeding and breast development
  - In boys presenting with acne, body odor, pubic hair and penile enlargement ^[3]
  - Both genders with gonadal pathologies ^[3]
- Fibrous dysplasia leading to pathologic fractures or pain ^[1] because of fibrous tissue replacing the normal bone ^[2]
  - This can be either monostotic (involving one bone) or polyostotic (involving multiple bones) ^[2]
- Café au lait spots with “coast of Maine” irregular borders ^[1] and are often the first presenting sign ^[2]
- Possible hyperthyroidism, Cushing syndrome, acromegaly or prolactin secretion due to increased thyroid, cortisol, growth hormone or prolactin secretion respectively depending on which tissues are affected ^[1]
- Phosphate wasting with or without hypophosphatemia ^[2] mediated by Fibroblast growth factor 23 (FGF23) ^[2]

Physical Examination

Patients with McCune-Albright syndrome usually present with bone pain or limping.
Physical examination may be remarkable for:
- Facial asymmetry due to craniofacial fibrous dysplasia
- Hearing impairment or visual disturbances due to craniofacial fibrous dysplasia
- Café au lait macules
- Goiter due to hyperthyroidism
- Macrocephaly due to excess growth hormone
- Vaginal bleeding in females due to ovarian cysts
- Pubic and or axillary hair and penile enlargement in males
- Growth acceleration in both genders
- Cushingoid features due to hypercortisolism

Laboratory Findings

Girls will have raised estradiol levels indicating an activated hypothalamic-pituitary axis.
Other laboratory findings consistent with the diagnosis of McCune-Albright syndrome are elevated growth hormone which can be deduced by an oral glucose tolerance test, serum GH and prolactin measurements.
Evaluation of hyperthyroidism is indicated by measuring TSH, free and bound thyroxine and T3. ^[1]

Electrocardiogram

There are no ECG findings associated with McCune-Albright syndrome.

X-ray

The fibrous dysplasia of bone is present at multiple sites (polyostotic) and xrays would give a ground glass appearance. ^[3]

Echocardiography or Ultrasound

US in boys may be helpful in the diagnosis of McCune-Albright syndrome. Findings on an US suggestive of McCune-Albright syndrome include testicular ultrasounds to identify hormonally active tumors.^[1]

CT scan

CT scan may be helpful in the diagnosis of McCune-Albright syndrome. Findings on CT scan suggestive of/diagnostic of McCune-Albright syndrome include fibroblastic lesions. It is helpful to identify these early in children to prevent permanent deformities. ^[1]

MRI

There are no MRI findings associated with McCune-Albright syndrome.

Other Imaging Findings

There are no other imaging findings associated with McCune-Albright syndrome.

Other Diagnostic Studies

McCune Albright may be diagnosed using total body bone scintigraphy to identify the fibrous dysplastic lesions. This should then be followed up with radiographs and CT to clearly determine the extent of the lesions. ^[2]
It is helpful to perform baseline ophthalmic and audiologic testing for those patients whose fibrous dysplastic lesions involve the craniofacial area ^[2]

Treatment

Medical Therapy

The treatment for McCune Albright syndrome includes:
- Precocious puberty- treatment is aimed to prevent bone age advancement ^[2]
  - For girls- Letrozole (aromatase inhibitor) and or tamoxifen (estrogen receptor modulator) ^[3]
  - For boys- treatment options are less well established ^[2]
- Fibrous dysplasia – treatment is aimed to minimize morbidity related to pain and fractures: ^[2]
  - Bisphosphonates such as zoledronic acid and pamidronate ^[2] have been used for fibrous dysplasia pain. ^[3]
- Endocrinopathies
  - Thyroid disease – Methimazole is effective though surgery is preferred ^[2]
  - Increased growth hormone
    - Octeotride which acts as a somatostatin analog and should be monitored for signs and symptoms of gallbladder disease ^[2]
    - Pegvisomant which is a growth hormone receptor antagonist and should be monitored for hepatotoxicity ^[2]
  - Hypercortisolism - metyparone is effective
  - FGF23-mediated phosphate wasting with oral phosphorus and calcitriol ^[2]

Surgery

Surgery should be used in extreme caution for female patients with ovarian cysts because of the high risk of recurrence and resultant decrease in ovarian reserve. ^[2]
Patients with hyperthyroidism are preferred to have a thyroidectomy with total gland resection ^[2]

Prevention

Once diagnosed patients with McCune-Albright syndrome are followed-up with:
- Females – early breast cancer screening ^[2]
- Males – testicular lesions by physical examination and US ^[2]
- Both genders – signs of precocious puberty, growth hormone excess or growth acceleration (IGF-1 levels), monitoring thyroid function (TSH, free T4, and T3), routine radiographs for fibrous dysplasia lesions particularly to check for scoliosis, serum phosphorous to monitor for development of hypophosphatemia ^[2] and annual vision and hearing testing to monitor fibrotic lesions affecting these areas. ^[1]
- Parents should be counseled that McCune-Albright syndrome is not inherited ^[2]
There is an increased risk for malignancies and it is advised to minimize radiation exposure and monitor patients regularly. ^[2]
Patients should also be advised to avoid contact sports and optic nerve decompressions ^[2]

References

↑ ^1.00 ^1.01 ^1.02 ^1.03 ^1.04 ^1.05 ^1.06 ^1.07 ^1.08 ^1.09 ^1.10 "StatPearls". 2020. PMID 30725777.
↑ ^2.00 ^2.01 ^2.02 ^2.03 ^2.04 ^2.05 ^2.06 ^2.07 ^2.08 ^2.09 ^2.10 ^2.11 ^2.12 ^2.13 ^2.14 ^2.15 ^2.16 ^2.17 ^2.18 ^2.19 ^2.20 ^2.21 ^2.22 ^2.23 ^2.24 Adam MP, Ardinger HH, Pagon RA, Wallace SE, Bean LJH, Stephens K; et al. (1993). "GeneReviews®". PMID 25719192.
↑ ^3.0 ^3.1 ^3.2 ^3.3 ^3.4 Pratt VM, McLeod HL, Rubinstein WS, Scott SA, Dean LC, Kattman BL; et al. (2012). "Medical Genetics Summaries". PMID 28520344.

External links

it:Sindrome di McCune-Albright-Sternberg

Template:WH Template:WikiDoc Sources

[pmid30725777-1] 1.00 ^1.01 ^1.02 ^1.03 ^1.04 ^1.05 ^1.06 ^1.07 ^1.08 ^1.09 ^1.10 "StatPearls". 2020. PMID 30725777.

[pmid25719192-2] 2.00 ^2.01 ^2.02 ^2.03 ^2.04 ^2.05 ^2.06 ^2.07 ^2.08 ^2.09 ^2.10 ^2.11 ^2.12 ^2.13 ^2.14 ^2.15 ^2.16 ^2.17 ^2.18 ^2.19 ^2.20 ^2.21 ^2.22 ^2.23 ^2.24 Adam MP, Ardinger HH, Pagon RA, Wallace SE, Bean LJH, Stephens K; et al. (1993). "GeneReviews®". PMID 25719192.

[pmid28520344-3] 3.0 ^3.1 ^3.2 ^3.3 ^3.4 Pratt VM, McLeod HL, Rubinstein WS, Scott SA, Dean LC, Kattman BL; et al. (2012). "Medical Genetics Summaries". PMID 28520344.

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[2]

[3]

v t e Congenital malformations and deformations of musculoskeletal system (Q65-Q79, 754-756)
Limbs	hip: Dislocation of hip/Hip dysplasia - Upington disease feet (Club foot, Flat feet, Pes cavus) systemic dislocations Larsen syndrome head, face, spine and chest: skull, face and jaw (Dolichocephaly, Greig cephalopolysyndactyly syndrome, Plagiocephaly) - spine Scoliosis - chest (Pectus excavatum, Pectus carinatum) any combination head, face, jaw, upper limb, lower limb, pelvis, dactyly Antley-Bixler syndrome - Schmitt Gillenwater Kelly syndrome dactyly Polydactyly/Syndactyly (Webbed toes) - Cenani Lenz syndactylism reduction deficits (Acheiropodia, Amelia, Ectrodactyly, Phocomelia) upper limb (Cleidocranial dysostosis, Madelung's deformity, Sprengel's deformity, Wallis Zieff Goldblatt syndrome) knee (Genu valgum, Genu varum) other Arthrogryposis
Skull and facial bones	Carpenter syndrome - Craniodiaphyseal dysplasia - Craniosynostosis (Scaphocephaly) - Crouzon syndrome - Hypertelorism - Macrocephaly - Oxycephaly - Platybasia - Saethre-Chotzen syndrome - Treacher Collins syndrome - Trigonocephaly
Spine and bony thorax	Klippel-Feil syndrome - Spondylolisthesis - Cervical rib - Bifid rib
Osteochondrodysplasia	developement of cartilage, tubular bones and spine: Achondrogenesis/Hypochondrogenesis - Boomerang dysplasia - Thanatophoric dysplasia - Short rib-polydactyly syndrome - Chondrodysplasia punctata (Rhizomelic chondrodysplasia punctata, Conradi-Hünermann syndrome), Achondroplasia (Hypochondroplasia, Osteosclerosis congenita) - Ellis-van Creveld syndrome - Otospondylomegaepiphyseal dysplasia - Spondyloepiphyseal dysplasia congenita - Osteogenesis imperfecta - McCune-Albright syndrome - Osteopetrosis - Metaphyseal dysplasia - Recessive multiple epiphyseal dysplasia - Hereditary multiple exostoses - Osteopoikilosis - Chondrodystrophy - Osteodystrophy - Atelosteogenesis, type II - Diastrophic dysplasia
Other	abdominal wall (Congenital diaphragmatic hernia, Omphalocele, Gastroschisis, Prune belly syndrome) - Ehlers-Danlos syndrome
See also non-congenital conditions (M, 710-739)