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Paraneoplastic Β· AutoimmuneICD-10 M33

Paraneoplastic dermatomyositis

Cancer-associated dermatomyositis; "malignancy-associated DM"; the paraneoplastic subgroup within the broader spectrum of idiopathic inflammatory myopathies

Dermatomyositis (DM) is an autoimmune inflammatory myopathy with characteristic cutaneous features β€” the heliotrope rash, Gottron papules and Gottron sign, the V sign, the shawl sign, holster sign and mechanic's hands β€” accompanied by symmetrical proximal muscle weakness and a wide range of pulmonary, cardiac and gastrointestinal complications. The skin-oncology importance lies in the substantially elevated cancer risk in adult-onset DM: in pooled studies, ~15–30% of adults with DM have an underlying or subsequently diagnosed malignancy, with a relative risk of ~6–8 over the general population. The risk is markedly higher in older patients (>50), male sex, certain myositis-specific autoantibodies (especially anti-TIF1-Ξ³), severe cutaneous disease and refractory myopathy. The classical malignancies are ovarian, lung, breast, colorectal and gastric carcinomas in Western populations, with nasopharyngeal carcinoma over-represented in East Asian populations. Comprehensive cancer screening at DM diagnosis and during the subsequent 3 years is now standard practice; the IMACS 2023 (Oldroyd et al., Nat Rev Rheumatol 2023) guidelines provide a structured approach.

CurrentLast reviewed 26 April 2026

Cutaneous features

  • Heliotrope rash β€” violaceous discolouration of the upper eyelids Β± periorbital oedema; pathognomonic.
  • Gottron papules β€” violaceous flat-topped papules over the dorsal MCP, PIP and DIP joints; pathognomonic.
  • Gottron sign β€” symmetric violaceous macules over the extensor surfaces of elbows, knees, malleoli (without papules).
  • V sign β€” V-shaped photo-distributed erythema on the upper anterior chest.
  • Shawl sign β€” erythema across the upper back and shoulders.
  • Holster sign β€” erythema on the lateral hips / thighs.
  • Mechanic's hands β€” hyperkeratotic fissured skin on lateral fingers and palms; particularly with anti-synthetase syndrome.
  • Periungual telangiectasia with cuticular hypertrophy ("ragged cuticles").
  • Calcinosis cutis β€” particularly in juvenile DM but also adult.
  • Diffuse poikiloderma in chronic disease.
  • Severe pruritus is common.

Cancer risk in adult-onset DM

  • ~15–30% of adults with DM have an associated malignancy (at diagnosis or within ~3 years).
  • Relative risk ~6–8 over the general population.
  • Risk highest in:
    • Older patients (>50).
    • Male sex.
    • Anti-TIF1-Ξ³ antibody positive β€” strongest single autoantibody marker (~70% of TIF1-Ξ³-positive adults have an underlying cancer at diagnosis or within 3 years).
    • Anti-NXP-2 antibody β€” second strongest autoantibody marker (especially in men).
    • Severe cutaneous disease.
    • Refractory myopathy.
    • Rapid onset.
    • Skin necrosis.
    • Dysphagia (oesophageal) β€” also a sign of severe DM.
  • The risk is concentrated in the 3 years before and after DM diagnosis.
  • Common underlying malignancies (Western populations):
    • Ovarian (women) β€” over-represented.
    • Lung.
    • Breast.
    • Colorectal.
    • Gastric.
    • Pancreatic.
    • Non-Hodgkin lymphoma.
  • East Asian populations β€” nasopharyngeal carcinoma (NPC) is the dominant association.

Cancer screening β€” IMACS 2023 (Oldroyd et al., Nat Rev Rheumatol 2023) guidelines

  • Risk-stratified approach based on autoantibody status, age, sex and risk factors.
  • Standard initial screen for all adults with new DM:
    • Full history and examination.
    • FBC, U&E, LFT, calcium, ESR / CRP.
    • Urinalysis.
    • Stool occult blood test / FIT.
    • Tumour markers β€” SCC antigen, CEA, CA19-9, CA15-3, CA125, AFP, PSA (guided by symptoms / sex).
    • Mammography (women); cervical screening up to date.
    • CT chest, abdomen, pelvis.
    • Pelvic MRI (women) β€” particularly important for ovarian carcinoma.
    • Upper GI endoscopy and colonoscopy in selected patients.
    • Nasopharyngoscopy in East Asian patients.
    • Whole-body PET-CT β€” increasingly used as a comprehensive single-test approach.
  • Repeat screening at 6, 12, 24 and 36 months in high-risk patients (anti-TIF1-Ξ³-positive, refractory disease, >50 years).
  • Refer to a rheumatology / connective tissue MDT.

Management

  • Treat the underlying malignancy β€” DM frequently improves with successful cancer treatment and may relapse with cancer recurrence.
  • Immunosuppression for the DM:
    • High-dose oral corticosteroid (prednisolone 1 mg/kg/day with slow taper).
    • Methotrexate or azathioprine β€” first-line steroid-sparing.
    • IVIg, mycophenolate, ciclosporin, tacrolimus β€” second-line.
    • Rituximab for refractory disease.
    • JAK inhibitors (tofacitinib, baricitinib) β€” emerging.
  • Photoprotection β€” DM eruption is photosensitive.
  • Topical corticosteroid / calcineurin inhibitor for skin disease.
  • Hydroxychloroquine for cutaneous DM.
  • Anti-pruritic measures β€” antihistamines, gabapentin / pregabalin.
  • Calcinosis cutis β€” challenging; topical sodium thiosulfate, surgical excision.
  • Refer to rheumatology, dermatology, respiratory medicine, oncology MDTs.

References

  1. Oldroyd AGS et al. International Guideline for Idiopathic Inflammatory Myopathy-associated Cancer Screening β€” IMACS / ENMC. Nat Rev Rheumatol; 2023.
  2. Trallero-AraguΓ‘s E et al. Cancer-associated myositis and antitif1Ξ³ antibody β€” review. Arthritis Rheum; 2012.

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