Dermatomyositis

Introduction[edit | edit source]

Erythematous papules overlying the MCP and IP joints

Dermatomyositis is an autoimmune inflammatory myositis, possibly related condition to polymyositis.^[1] It is characterized by inflammatory and degenerative changes in the muscles and skin leading to symmetric weakness and some degree of muscle atrophy, principally in the limb girdles, neck and pharynx.  This disease has also shown to effect the esophagus, lungs, and least commonly the heart. Also classified in the umbrella term Inflammatory Myopathies.^[2][3][4] 

Epidemilogy[edit | edit source]

Female predilection. Bimodal age pattern: Juvenile dermatomyositis (JDM), affects children and is more severe; Adult dermatomyositis (ADM) usually affects adults around the age of 50.^[1]

Etiology[edit | edit source]

The cause of dermatomyositis is unknown, however several genetic, immunologic, and environmental factors are implicated in this condition.^[5]

Characteristics/Clinical Presentation[edit | edit source]

Classically presents with a symmetrical proximal myopathy with associated dermatological changes including, dusky-red rash over the face, arms, hands, legs and other features. Other features include, dysphagia, myalgia, fever and weight loss^[1].

• Muscle weakness: that starts slowly and worsens over time. It first affects proximal muscles symmetrically, with distal muscles becoming involved later. This results in difficulties with everyday activities like standing up, climbing stairs, or lifting objects. Severe cases can lead to head drop, difficulty swallowing and speaking, and weakened breathing muscles. While less common, some patients may also experience muscle pain and tenderness.
• Skin disease: dermatomyositis (DM) is characterized by a rash it can appear before, alongside, or after muscle weakness the key skin features may include: ^[6]
  • Gottron's papules: Erythematous to violaceous bumps on the knuckles, potentially with scaling and ulceration, leading to scarring.
  • Gottron's sign: Erythematous patches on elbows and knees (less specific).
  • Heliotrope rash: Purple eyelid erythema with swelling and tiny blood vessels (telangiectasia), sometimes subtle in darker skin.
  • Erythematous patches in sun-exposed and non-sun-exposed areas.
  • Malar erythema: Redness across cheeks, extending to the nose and nasolabial folds.
  • "V" sign: Confluent redness on the lower neck and upper chest.
  • Shawl sign: Erythema on the upper back, neck, and shoulders, possibly extending to the arms.
  • Scalp involvement and skin issues on the lower back and lateral thighs (Holster sign).
  • Rarely, extensive erythroderma covering more than 50% of the body surface or a severe, cracked skin variant can occur.

Systemic Involvement[edit | edit source]

Systemic manifestations:
Common: proximal muscle weakness, dysphonia, dysphagia
Less common: respiratory muscle weakness, visual changes, abdominal pain

Systemic complications/association:

Aspiration pneumonia secondary to respiratory muscle weakness
Diffuse interstitial pneumonitis/fibrosis
Large-bowel infarction secondary to vasculopathy has occurred in juvenile patients with myositis
Muscle atrophy
Muscle calcification
Ocular complications including iritis, nystagmus, cotton-wool spots, optic atrophy, conjunctival edema and pseudopolyposis
Internal malignancy
Cardiomyopathy Cardiac conduction defects^[7]

Complications Malignancy[edit | edit source]

There is a six fold increased risk of malignancy in dermatomyositis. This risk appears to be highest in patients diagnosed with dermatomyositis after 45 years of age. Risk factors include: >60 years old; male; dysphagia; necrosis of the skin; cutaneous vasculitis; accelerated onset of disease; increased creatine kinase (CK) levels; increased ESR and C-reactive protein (CRP) levels^[8].

Diagnostic Tests/Lab Tests/Lab Values[edit | edit source]

laboratory studies are helpful but nonspecific:

•  ESR frequently elevated
•  Antinuclear antibodies (ANA) elevated in 60 to 80 percent of patients
•  Elevated creatine kinase (CK) enzyme, transaminases, and lactate dehyrogenase levels
•  EMG to measure the electrical activity of the muscles: typically present as short-wave and fibrillations or myopathic pattern, 10 percent are false-negative
• Rheumatoid factor: elevated in 20 percent of patients, most often in those with overlap syndromes
• Neopterin and factor VIII–related antigen (von Willebrand factor): reported to correlate with juvenile DM^[7][4]

Management[edit | edit source]

The goals of managing dermatomyositis are focused on treating muscle weakness, skin disease, and addressing any other underlying complications. Physical therapy and rehabilitation play an essential role in management. ^[5] The treatment regimen must be instituted early and requires a team approach between the physical therapist, dermatologist and family physician.  While currently there is no cure for this systemic disease the symptoms can be treated.  Corticosteroids are used initially to reduce the inflammation, shorten the time to normalization of muscle enzymes, and reduce morbidity. Maintenance therapy with Prednisone usually is necessary indefinitely in the adult patient. Immunosuppressive therapies may be used in individuals who do not respond well to the corticosteroids.  The skin disease is primarily treated with sun avoidance, topical corticosteroids, antimalarial agents,methotrexate, mycophenolate mofetil, and/or intravenous immune globulin.  Patient education is highly important to assist in control of the disease process.^[4][7]

Physical Therapy Management[edit | edit source]

Patients with mild disease should be encouraged to engage in active exercise programs. Range of motion exercises help in preventing contractures. Patients with esophageal dysfunction may require elevation of the head off the bed, thickening of feeds, and even feeding via gastric tubes when indicated.^[5]

Focus of Treatment should include: 

• Strengthening to prevent atrophy once inflammation is controlled
• Range of motion exercises to prevent contractures
• Passive stretching and splinting^[7][9]
  

Differential Diagnosis^[10][edit | edit source]

• CREST Syndrome
• Parapsoriasis
• Graft Versus Host Disease
• Pityriasis Rubra Pilaris
• Lichen Myxedematosus
• Polymorphous Light Eruption
• Lichen Planus
• Psoriasis, Plaque
• Lupus Erythematosus, Acute
• Rosacea
• Lupus Erythematosus, Discoid
• Sarcoidosis
• Lupus Erythematosus, Subacute Cutaneous
• Tinea Corporis
• Morphea
• Urticaria, Chronic
• Multicentric Reticulohistiocytosis
  

References[edit | edit source]