PHACE syndrome

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PHACE Syndrome
Other namesPascual–Castroviejo type II syndrome, P-CIIS, Pascual–Castroviejo syndrome type 2 [1]
Specialty Medical genetics   OOjs UI icon edit-ltr-progressive.svg

PHACE syndrome is a medical condition characterized by uncommon associations between birth defects of the brain, skin (large facial infantile hemangiomas), arteries, heart and eyes. "PHACE" is an acronym for the parts of the body the syndrome usually impacts:

Contents

Sometimes an "S" is added to PHACE making the acronym PHACES; with the "S" standing for "Sternal defects" and/or "Supraumbilical raphe." PHACE syndrome may affect infants with large plaque-type facial hemangiomas. [3] Children who present this skin condition should receive careful ophthalmologic, cardiac, and neurologic assessment. According to one study of infants with large hemangiomas, one-third have symptoms consistent with the diagnosis of PHACE syndrome. The most common are cerebrovascular and cardiovascular anomalies. [4]

Signs and symptoms

Hemangiomas associated with PHACE syndrome are generally small or not visible at birth, but often escalate after days or weeks, gradually becoming easier to see. They also tend to cover a large area of the face, head, or neck, either as one lesion or as many individual lesions.

Patients with PHACE syndrome may also experience symptoms such as:

Cause and complications

Cause

The cause of PHACE syndrome is currently unknown. Researchers believe that it is caused by a postzygotic somatic mosaic mutation, or a mutation that can occur on any autosomal chromosome. Research is complicated due to the mosaic nature of the disease. [5] The disorder may be caused by genetic factors, environmental factors, or a combination of the two. [6]

Complications

As it grows, the hemangioma can break down the skin, distort facial features, or get in the way of other vital functions, such as breathing, vision, and hearing. Further complications will depend on what other structures are involved. These could include developmental delay, seizures, headaches, and abnormal muscle tone if the brain is affected.

Diagnosis

Since the initial sign of PHACE syndrome is usually a large facial hemangioma, infants born with this condition should be further evaluated to diagnose or rule out PHACE syndrome through a series of radiologic tests such as magnetic resonance images (MRI) or magnetic resonance angiograms (MRA) of the head, neck, and chest. Following the imaging tests, the physician should perform an echocardiogram on the infant to observe any abnormalities. If abnormalities are detected on these scans, the infant may have PHACE syndrome. [7]

Treatment

Due to the disorder's rarity, there are no standardized treatment protocols or guidelines and no medical treatment trials for affected individuals as of 2022. Various treatments have been reported in the medical literature as part of single case reports or small series of patients. [8]

Physicians treat specific complications and effects of the disorder in order to improve the lives of patients. Treatment usually involves collaboration between many medical professionals. These medical professionals include, but are not limited to, dermatologists; ophthalmologists; cardiologists; endocrinologists; neurologists and or neurosurgeons; otolaryngologists; dentists; speech pathologists; psychiatrists; and many others. [9]

Management

PHACE syndrome needs to be managed by a multidisciplinary team of experts. Additional specialties such as cardiology, ophthalmology, neurology, and neurosurgery may need to be involved. The experts pay close attention to how these children develop throughout school-age. [10] [11]

Since the establishment of the PHACE syndrome community non-profit in 2013, it has been raising awareness about the condition, supporting patients and families of those with the disease, and raising money for research into causes and treatment.

History

In 1993, a correlation between large facial hemangiomas and brain defects among 9 subjects was reported. [12] 3 years later, a larger case study was published showing a wider spectrum of grouped malformations. [13] The association of anomalies and the PHACES acronym was first coined by Dr. Vail Reese and Dr. Ilona Frieden in 1996, making it a newly described syndrome. A diagnosis is generally made from the physical examination, along with imaging of the head and chest, and an eye examination. PHACE is most commonly diagnosed among female infants. Long-term quality of life varies.

The hemangioma growth phase can last anywhere from 6 to 18 months. Then involution, or healing, of the hemangioma begins. Laser and other surgeries can usually make a substantial positive impact on appearance. Long after the hemangioma recedes, any damage it or the other defects caused may remain. Migraines are common, as are developmental delays.

See also

Related Research Articles

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A hemangioma or haemangioma is a usually benign vascular tumor derived from blood vessel cell types. The most common form, seen in infants, is an infantile hemangioma, known colloquially as a "strawberry mark", most commonly presenting on the skin at birth or in the first weeks of life. A hemangioma can occur anywhere on the body, but most commonly appears on the face, scalp, chest or back. They tend to grow for up to a year before gradually shrinking as the child gets older. A hemangioma may need to be treated if it interferes with vision or breathing or is likely to cause long-term disfigurement. In rare cases internal hemangiomas can cause or contribute to other medical problems. They usually disappear in 10 years. The first line treatment option is beta blockers, which are highly effective in the majority of cases. Hemangiomas that form at birth are called congenital hemangiomas, while those that form later in life are called infantile hemangiomas.

Diffuse capillary malformation with overgrowth (DCMO) is a subset of capillary malformations (CM) associated with hypertrophy, i.e. increased size of body structures. CM can be considered an umbrella term for various vascular anomalies caused by increased diameter or number of capillary blood vessels. It is commonly referred to as "port-wine stain", and is thought to affect approximately 0.5% of the population. Typically capillaries in the papillary dermis are involved, and this gives rise to pink or violaceous colored lesions. The majority of DCMO lesions are diffuse, reticulated pale-colored stains.

References

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  4. Haggstrom, AN; Garzon, MC; Baselga, E; Chamlin, SL; Frieden, IJ; Holland, K; Maguiness, S; Mancini, AJ; McCuaig, C; Metry, DW; Morel, K; Powell, J; Perkins, SM; Siegel, D; Drolet, BA (2010). "Risk for PHACE syndrome in infants with large facial hemangiomas". Pediatrics. 126 (2): e418–26. doi:10.1542/peds.2009-3166. PMID   20643720. S2CID   25928589.
  5. Thorpe, Jeremy; Osei-Owusa, Ikeoluwa; Erlanger Avigdor, Bracha; Tupler, Rossella; Pevsner, Jonathan (2022-09-11). "Mosaicism in Human Health and Disease". Annual Review of Genetics. 54: 487–510. doi:10.1146/annurev-genet-041720-093403. PMC   8483770 . PMID   32916079.
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  7. "PHACE syndrome". Children's Hospital of Wisconsin. Retrieved 2018-10-25.
  8. Lanes, Marsha. "PHACE Syndrome". NORD (National Organization for Rare Disorders). Retrieved 2022-07-11.
  9. "PHACE Syndrome - NORD (National Organization for Rare Disorders)". NORD (National Organization for Rare Disorders). Retrieved 2018-10-25.
  10. "PHACE Syndrome Community".
  11. Drolet, Beth. "PHACE Syndrome handbook". Children's Hospital of Wisconsin. Archived from the original on 16 July 2016. Retrieved 6 June 2022.
  12. Reese, V; Frieden, IJ; Paller, AS; Esterly, NB; Ferriero, D; Levy, ML; Gellis, SE; Siegfried, EC (March 26, 1993). "Association of facial hemangioma with Dandy-Walker and other posterior fossa malformations". Journal of Pediatrics. 122 (3): 379–384. doi:10.1016/s0022-3476(05)83420-1. PMID   8441091 . Retrieved 10 October 2016.
  13. Frieden, IL; Reese, V; Cohen, D (Mar 1996). "PHACE syndrome. The association of posterior fossa brain malformations, hemangiomas, arterial anomalies, coarctation of the aorta and cardiac defects, and eye abnormalities". Archives of Dermatology. 132 (3): 307–311. doi:10.1001/archderm.132.3.307. PMID   8607636.