Dermatomyositis.

Dermatomyositis is a rare autoimmune disease causing inflammation of muscle and skin. Patients develop symmetric proximal muscle weakness, a violaceous rash on the eyelids (heliotrope), and Gottron papules over the knuckles, elbows, and knees. It can also affect the lungs, heart, and oesophagus.

Early signs include a violaceous discolouration of the upper eyelids, a photosensitive rash over the chest and shoulders, and progressive difficulty climbing stairs, rising from chairs, or lifting arms above the head. Skin signs often precede muscle symptoms by weeks to months.

Yes. About 15-25% of adult cases have an underlying malignancy diagnosed within 3 years of dermatomyositis. Anti-TIF1-gamma antibody is the strongest predictor. Annual cancer screening (CT, mammography, gynaecological exam, colonoscopy, tumour markers) is recommended for 3 years after diagnosis.

Diagnosis uses the 2017 EULAR/ACR criteria combining characteristic skin signs, proximal muscle weakness, elevated muscle enzymes, abnormal EMG, MRI muscle oedema, and biopsy showing perifascicular atrophy. Myositis-specific antibodies (Mi-2, MDA5, TIF1-gamma, NXP2, SAE, synthetases) define the clinical subset.

First-line treatment is oral prednisolone 0.75-1 mg/kg/day combined with methotrexate or mycophenolate mofetil. Intravenous immunoglobulin is now widely used as a steroid-sparing agent based on the ProDERM trial. Rituximab and JAK inhibitors are reserved for refractory or severe disease.

Dermatomyositis is not curable but can be brought into long remission with treatment. About 60-80% of adults achieve substantial improvement on combination immunosuppression. Most patients need long-term low-dose maintenance therapy. Cancer-associated cases often improve when the underlying tumour is treated.

Anti-MDA5 dermatomyositis is a clinically amyopathic subtype with little muscle disease but a high risk of rapidly progressive interstitial lung disease, especially in East Asian patients. It carries 1-year mortality up to 40-60% without intensive triple therapy combining steroids, calcineurin inhibitors, and JAK inhibitors or rituximab.

Heliotrope rash is a violaceous (lilac-coloured) discolouration of the upper eyelids, sometimes with periorbital swelling. It is named after the colour of the heliotrope flower. It is pathognomonic for dermatomyositis when seen with proximal muscle weakness or Gottron papules.

Gottron papules are pink-purple, flat-topped papules over the dorsal metacarpophalangeal and interphalangeal joints, and sometimes elbows, knees, or medial malleoli. They are pathognomonic for dermatomyositis and often accompany the heliotrope rash and proximal muscle weakness.

Yes. Juvenile dermatomyositis is the most common idiopathic inflammatory myopathy in childhood, with peak onset at age 5-15 years. Cancer association is much lower than in adults. Calcinosis cutis is more common but long-term outcomes are generally favourable with early aggressive treatment.

Intravenous immunoglobulin given as 2 g/kg every 4 weeks improves muscle strength, skin disease, and dysphagia. The ProDERM phase 3 trial (NEJM 2022) showed significant improvement in 79% of IVIG patients versus 44% on placebo at 16 weeks, with benefit sustained at 40 weeks.

Yes. Ultraviolet light exposure precipitates and worsens cutaneous disease. Patients should use SPF 50+ broad-spectrum sunscreen daily, UV-protective clothing, and avoid midday sun. Photoprotection often reduces the need for higher-dose immunosuppression.

Yes. Interstitial lung disease affects 20-40% of adult dermatomyositis patients and is the main cause of mortality. Anti-MDA5 antibody predicts rapidly progressive ILD; anti-synthetase antibodies predict chronic ILD. High-resolution CT and pulmonary function tests are essential at diagnosis.

Yes. Once acute inflammation is controlled, supervised aerobic and resistance exercise improves strength, function, and quality of life. Gentle range-of-motion exercises during the acute phase prevent contractures and deconditioning. Avoid sun exposure during outdoor exercise.

Calcinosis cutis is calcium deposition in skin, subcutaneous tissue, and sometimes muscle, leading to firm nodules, chronic ulcers, and secondary infection. It affects 30-70% of juvenile and 10-20% of adult cases. Treatments include diltiazem, bisphosphonates, sodium thiosulphate, and surgical excision for severe cases.

Statins can rarely trigger a dermatomyositis-like syndrome or worsen pre-existing disease. They should be reviewed at diagnosis and stopped if a temporal association is suspected. Hyperlipidaemia from steroid therapy may still need treatment with alternative agents.

Yes. Relapses occur in 30-50% of patients within 5 years, often when immunosuppression is reduced. Monitoring muscle enzymes, skin signs, and myositis-specific antibody titres detects relapse early. Restarting or escalating immunosuppression usually regains control.

Five-year survival in adult dermatomyositis without ILD or cancer is now 80-90%, and 95% in juvenile disease. Anti-MDA5 with rapidly progressive ILD and cancer-associated disease have substantially worse prognosis. Cardiovascular disease, infection, and malignancy are leading competing risks long-term.

There is a genetic susceptibility component (HLA-DRB1*0301, HLA-DRB1*0701, and several immune-regulatory loci), but the disease is not directly inherited. Most cases are sporadic. Family members rarely develop dermatomyositis themselves but may have other autoimmune conditions.

Yes, when the disease is in remission for at least 6 months on pregnancy-safe medications (hydroxychloroquine, azathioprine, low-dose steroids, IVIG). Mycophenolate and methotrexate are teratogenic and must be stopped 3 months before conception. Multidisciplinary care improves outcomes.

All adults with new dermatomyositis should have age-appropriate cancer screening at diagnosis — chest, abdominal, and pelvic CT, mammography, gynaecological exam, colonoscopy if indicated, and tumour markers. Repeat screening every 6-12 months for at least 3 years, when cancer risk is highest.