Oculopharyngeal Muscular Dystrophy

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Retrieved

2021-01-23

Source

Orphanet

Trials

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Genes

PABPN1, LRP12, NUTM2B-AS1, GCG, PABPC1P2, BCL2L2-PABPN1, NRL, PABPC1, SACS, TNNT3, TARDBP, SIRT1, SYNM, SIRT2, OPTN, DNAJB6, GCA, BCL2, TGM2, CTNNB1, PRKAB1, PRKAA2, PRKAA1, PAX7, MLF1, LTBP3, IL6, DNAJA1, HNRNPA2B1, HNRNPA1

Drugs

Trehalose, genetically modified adeno-associated viral vector serotype 9 expressing shRNA as well as a codon-optimised shRNA-insensitive wildtype PABPN1

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Oculopharyngeal muscular dystrophy (OPMD) is an adult-onset progressive myopathy characterized by progressive eyelid ptosis, dysphagia, dysarthria and proximal limb weakness.

Epidemiology

OPMD is seen worldwide with varying prevalence rates. The estimated prevalence rate in Europe is 1/200,000-1/100,000. The highest prevalence rate of 1/1,000 is found in French Canadians in Quebec and 1/600 in Israel's Bukharan Jews.

Clinical description

Disease onset occurs in the fifth to sixth decade of life. Early signs include ptosis, limb weakness and dysphagia. Symptoms usually begin after the age of 45 years, and ptosis is the most common presenting feature. Other signs that occur as the disease progresses include tongue weakness and atrophy, proximal upper and lower extremity weakness, dysphonia, dysarthria, facial muscle weakness, and limitation of upward gaze. In several cases, limb weakness has preceded dysphagia. In 5-10% of patients, the disease is more severe, with ptosis and dysphagia presenting before the age of 45 and incapacitating distal leg weakness occurring before the age of 60. The manifestations of autosomal recessive OPMD usually present later (after the age of 60) than those of the autosomal dominant form.

Etiology

OPMD is caused by an expansion of the polyalanine tract in the gene PABPN1 (14q11.2), which leads to overexpression of a mutant protein and consequently to the accumulation of nuclear aggregates in the muscles.

Diagnostic methods

OPMD is diagnosed by genetic confirmation of a mutation in the PABPN1 gene. Supportive evidence comes from finding tubulofilamentous inclusions in the nuclei of myocytes (intranuclear inclusions) using electron microscopy, as well as muscle fibers containing rimmed vacuoles, but a muscle biopsy is not needed for diagnosis. Creatine kinase (CK) levels are slightly elevated and electromyogram (EMG) studies may suggest a mild myopathic process.

Differential diagnosis

Differential diagnoses include oculopharyngodistal myopathy, myasthenia gravis, Steinert myotonic dystrophy, proximal myotonic myopathy, congenital fibrosis of extraocular muscles, blepharophimosis-epicanthus inversus-ptosis syndrome (see these terms), autosomal dominant distal myopathy, and mitochondrial myopathy.

Antenatal diagnosis

Prenatal diagnosis is possible, but as this condition presents in adulthood, it is very rarely performed.

Genetic counseling

OPMD is inherited both autosomal dominantly (in most cases) and recessively. Genetic counseling is possible when a PABPN1 mutation has been identified in a family.

Management and treatment

No pharmacological treatment is presently available, but surgical treatments are offered that can help with ptosis and dysphagia. A blepharoplasty can treat ptosis when the eyelids cover more than 50% of the pupils or when neck pain is present. A cricopharyngeal myotomy can be performed to achieve normal swallowing, but dysphagia usually recurs years after surgery. The intake of dietary supplements and a diet of foods that are soft and easy to swallow are often necessary. Some patients may need a wheelchair if muscle atrophy is severe.

Prognosis

Ptosis and dysphagia typically recur within five to fifteen years after surgery. There is usually no decrease in life expectancy, but quality of life can be reduced in those where the disease is debilitating. Death is usually due to aspiration pneumonia or malnutrition (with severe weight loss) in elderly patients.