Parry–Romberg syndrome (also known as progressive hemifacial atrophy) is a rare neurocutaneous syndrome characterized by progressive shrinkage and degeneration of the tissues beneath the skin, usually on only one side of the face (hemifacial atrophy) but occasionally extending to other parts of the body. An autoimmune mechanism is suspected, and the syndrome may be a variant of localized scleroderma, but the precise etiology and pathogenesis of this acquired disorder remains unknown. The syndrome has a higher prevalence in females and typically appears between 5 – 15 years of age.

In addition to the connective tissue disease, the condition is often accompanied by significant neurological, ocular and oral signs and symptoms. The range and severity of associated symptoms and findings are highly variable.

Signs and symptoms

Skin and connective tissues

Initial facial changes usually involve the area of the face covered by the temporal or buccinator muscles. The disease progressively spreads from the initial location, resulting in atrophy of the skin and its adnexa, as well as underlying subcutaneous structures such as connective tissue, (fat, fascia, cartilage, bones) and/or muscles of one side of the face.^[1] The mouth and nose are typically deviated towards the affected side of the face.^[2]

The process may eventually extend to involve tissues between the nose and the upper corner of the lip, the upper jaw, the angle of the mouth, the area around the eye and brow, the ear, and/or the neck.^[1][2] The syndrome often begins with a circumscribed patch of scleroderma in the frontal region of the scalp which is associated with a loss of hair and the appearance of a depressed linear scar extending down through the midface on the affected side. This scar is referred to as a "coup de sabre" lesion because it resembles the scar of a wound made by a sabre, and is indistinguishable from the scar observed in frontal linear scleroderma.^[3][4]

In 20% of cases, the hair and skin overlying affected areas may become hyperpigmented or hypopigmented with patches of unpigmented skin. In up to 20% of cases the disease may involve the ipsilateral (on the same side) or contralateral (on the opposite side) neck, trunk, arm, or leg.^[5] The cartilage of the nose, ear and larynx can be involved. The disease has been reported to affect both sides of the face in 5-10% of the cases.^[3]

Symptoms and physical findings usually become apparent during the first or early during the second decade of life. The average age of onset is nine years of age,^[1] and the majority of individuals experience symptoms before 20 years of age. The disease may progress for several years before eventually going into remission (abruptly ceasing).^[1]

Neurological

Neurological abnormalities are common. Roughly 45% of people with Parry–Romberg syndrome are also afflicted with trigeminal neuralgia (severe pain in the tissues supplied by the ipsilateral trigeminal nerve, including the forehead, eye, cheek, nose, mouth and jaw) and/or migraine (severe headaches that may be accompanied by visual abnormalities, nausea and vomiting).^[5][6]

10% of affected individuals develop a seizure disorder as part of the disease.^[5] The seizures are typically Jacksonian in nature (characterized by rapid spasms of a muscle group that subsequently spread to adjacent muscles) and occur on the side contralateral to the affected side of the face.^[1] Half of these cases are associated with abnormalities in both the gray and white matter of the brain—usually ipsilateral but sometimes contralateral—that are detectable on magnetic resonance imaging (MRI) scan.^[5][7]

Ocular

Enophthalmos (recession of the eyeball within the orbit) is the most common eye abnormality observed in Parry–Romberg syndrome. It is caused by a loss of subcutaneous tissue around the orbit. Other common findings include drooping of the eyelid (ptosis), constriction of the pupil (miosis), redness of the conjunctiva, and decreased sweating (anhidrosis) of the affected side of the face. Collectively, these signs are referred to as Horner's syndrome. Other ocular abnormalities include ophthalmoplegia (paralysis of one or more of the extraocular muscles) and other types of strabismus, uveitis, and heterochromia of the iris.^[8][9]

Oral

The tissues of the mouth, including the tongue, gingiva, teeth and soft palate are commonly involved in Parry–Romberg syndrome.^[2] 50% of affected individuals develop dental abnormalities such as delayed eruption, dental root exposure, or resorption of the dental roots on the affected side. 35% have difficulty or inability to normally open the mouth or other jaw symptoms, including temporomandibular joint disorder and spasm of the muscles of mastication on the affected side. 25% experience atrophy of one side of the upper lip and tongue.^[5]

Causes

The fact that some people affected with this disease have circulating antinuclear antibodies in their serum supports the theory that Parry–Romberg syndrome may be an autoimmune disease, specifically a variant of localized scleroderma.^[10] Several instances have been reported where more than one member of a family has been affected, prompting speculation of an autosomal dominant inheritance pattern. However, there has also been at least one report of monozygotic twins in which only one of the twins was affected, casting doubt on this theory. Various other theories about the etiology and pathogenesis have been suggested, including alterations in the peripheral sympathetic nervous system (perhaps as a result of trauma or infection involving the cervical plexus and/or the sympathetic trunk), disorders in migration of cranial neural crest cells, or chronic cell-mediated iflammatory process of the blood vessels. It is likely that the disease results from different mechanisms in different people, with all of these factors potentially being involved.^[1]

Diagnosis

Diagnosis can be made solely on the basis of history and physical examination in people who present with only facial asymmetry. For those who report neurological symptoms such as migraine or seizures, MRI scan of the brain is the imaging modality of choice. A diagnostic lumbar puncture and serum test for autoantibodies may also be indicated in people who present with a seizure disorder of recent onset.^[5]

Management

Medical

Medical management may involve immunosuppressive drugs such as methotrexate, corticosteroids, cyclophosphamide, and azathioprine. No randomized controlled trials have yet been conducted to evaluate such treatments, so the benefits have not been clearly established.^[5]

Surgical

Affected individuals may benefit from microsurgical reconstructive surgery to restore a more normal contour to the face. Such surgery often involves the transfer of an island parascapular fasciocutaneous flap or a free flap from the groin, rectus abdominis muscle (Transverse Rectus Abdominis Myocutaneous or "TRAM" flap) or latissimus dorsi muscle to the face. Severe deformities may require additional procedures, such as pedicled temporal fascia flaps, cartilage grafts, bone grafts, orthognathic surgery, and bone distraction.^[11] The timing of surgical intervention is controversial; some surgeons prefer to wait until the disease has run its course^[2] while others recommend early intervention.^[12]

Epidemiology

Parry–Romberg syndrome appears to occur randomly and for unknown reasons. Prevalence is higher in females than males, with a ratio of roughly 3:2. The condition is observed on the left side of the face about as often as on the right side.^[13]

History

The disease was first described in 1825 by Caleb Hillier Parry (1755 – 1822), in a collection of his medical writings which were published posthumously by his son Charles Henry Parry (1779 – 1860).^[14] It was described a second time in 1846 by Moritz Heinrich Romberg (1795 – 1873) and Eduard Heinrich Henoch (1820 – 1910).^[15] German neurologist Albert Eulenburg (1840 – 1917) was the first to use the descriptive title "progressive hemifacial atrophy" in 1871.^[16][17][18]

Additional Images

• A 3D, soft tissue reconstruction of a CT scan of a 17 year old girl with Parry Romberg syndrome.

• CT scan3D bone reconstruction of a 17 year old girl with Parry Romberg syndrome.

• Child affected by Parry Romberg syndrome

See also

• Hemifacial microsomia
• List of cutaneous conditions
• Trigeminal trophic lesion

References

Further reading

• Karim, A; Laghmari M, Ibrahimy W, Essakali HN, Mohcine Z (2005). "Neuroretinitis, Parry-Romberg syndrome, and scleroderma" (in French). Journal of French Ophthalmology 28 (8): 866–70. PMID 16249769.
• Lakhani, PK; David, TJ (1984). "Progressive hemifacial atrophy with scleroderma and ipsilateral limb wasting (Parry-Romberg syndrome)". Journal of the Royal Society of Medicine 77 (2): 138–9. PMC 1439690. PMID 6737396. //www.ncbi.nlm.nih.gov/pmc/articles/PMC1439690/.
• Larner, AJ; Bennison, DP (1993). "Some observations on the aetiology of progressive hemifacial atrophy ("Parry-Romberg syndrome")". Journal of Neurology, Neurosurgery and Psychiatry 56 (9): 1035–6. PMC 489747. PMID 8410030. //www.ncbi.nlm.nih.gov/pmc/articles/PMC489747/.
• Miller, MT; Spencer, MA (1995). "Progressive hemifacial atrophy. A natural history study". Transactions of the American Ophthalmological Society 93: 203–15. PMC 1312058. PMID 8719679. //www.ncbi.nlm.nih.gov/pmc/articles/PMC1312058/.
• Pinheiro, TP; Silva CC, Silveira CS, Botelho PC, Pinheiro MG, Pinheiro Jde J (2006). "Progressive Hemifacial Atrophy--case report". Med Oral Patol Oral Cir Bucal 11 (2): E112–4. PMID 16505785.
• Zafarulla, MY (1985). "Progressive hemifacial atrophy: a case report". British Journal of Ophthalmology 69 (7): 545–7. PMC 1040666. PMID 4016051. //www.ncbi.nlm.nih.gov/pmc/articles/PMC1040666/.

External links

• Progressive hemifacial atrophy; Parry-Romberg syndrome at NIH's Office of Rare Diseases
• The Romberg's Connection: an international support group for individuals and families whose lives are affected by Parry–Romberg syndrome
• Parry-Romberg Syndrome Resource: a nonprofit organization dedicated to providing awareness of Parry-Romberg Disease