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Editors
Discoid Lupus Erythematosus
- This article addresses the type of lupus erythematosus that is mainly confined to the skin (DLE). See also the article Systemic lupus erythematosus Systemic Lupus Erythematosus (Sle).
Essentials
- Photosensitivity may be due to DLE.
- Diagnosis is based on clinical presentation and histological examination of a skin biopsy.
- Management consists of symptomatic treatment and prevention of exacerbations.
- The possibility of systemic lupus erythematosus (SLE) should be considered.
- Cutaneous manifestations are encountered in all main types of lupus disease: DLE, subacute cutaneous lupus erythematosus (SCLE) and SLE.
Definition, aetiology and epidemiology
- A chronic photosensitive autoimmune disease, which may cause permanent scarring on the skin
- Aetiology is unknown but hereditary factors play a part in disease appearance.
- More common in women, age of onset generally between 20 and 40 years
Disease types
- In lupus confined to the skin, other clinical subtypes have been described in addition to the most common discoid (DLE) type.
- DLE must be differentiated from SLE, which is associated with systemic symptoms.
- SCLE is a subtype of DLE with reddish and scaly lesions mainly on the upper body and mild systemic symptoms (pictures 1 2).
- Overlapping is noted when only the cutaneous manifestations of lupus diseases are evaluated.
- 10-20% of patients with SLE present with cutaneous symptoms suggestive of DLE.
- 5-10% of patients with DLE may develop SLE with time.
- The different types of lupus diseases are distinguished with the aid of clinical presentation, systemic symptoms and laboratory investigations (antinuclear antibodies).
Clinical presentation
- Skin lesions are visible on areas exposed to the sun (face: pictures 3 4; scalp: pictures 5 6; neck, upper chest; backs of the hands, arms).
- DLE may have many clinical manifestations, and the course of the disease may be variable.
- Exacerbations are usually seen in the spring and summer.
- The typical plaques are clearly demarcated, the size of a finger tip, reddish and scaly; as they develop they may atrophy in the middle and scar the skin.
- The lesions are usually asymptomatic, but they may present with pruritus or tenderness.
- The lesions often develop 1-2 weeks after sunlight exposure.
- On the scalp, DLE may cause scarring alopecia (see Hair Loss and Balding), which may have significant aesthetic implications.
- Rarely causes ulceration in the oral mucosa (picture 7).
- Some patients exhibit systemic symptoms, such as fatigue, myalgia, arthralgia, slight fever and laboratory tests may show abnormalities (see below).
- In these cases, the symptomatology may overlap with that of SLE and other connective tissue disorders. The full criteria for SLE are usually not fulfilled.
Diagnosis
- Based on clinical presentation as well as histological and immunofluorescence tests of a skin biopsy
- Fungal samples (for culture and microbiology) of single lesions may be indicated to exclude tinea.
- SLE may produce similar skin lesions and must be excluded with the aid of patient history, physical examination and laboratory tests.
- Full blood count, CRP, ESR
- Creatinine, ALT, alkaline phosphatase
- Urinalysis
- Serum antinuclear antibody analysis, antibodies to extractable nuclear antigens, DNA antibodies
- Plasma C3 and C4 complement levels
- Any systemic symptoms are investigated using appropriate laboratory tests and imaging techniques.
- The results may be positive for antinuclear antibodies (the ANA test is positive in 5-10% of patients) and show blood picture changes (leucocytopenia, thrombocytopenia) even in cases where the disease is confined to the skin.
- Typical autoantibody profiles may be seen in connective tissue disorders.
- Diagnosis can never be made based on antibody tests alone, and overlapping between the diseases occurs.
- A positive test result for SSA antibodies and SSB antibodies (Sjögren's syndrome antibodies), may be suggestive of SCLE.
- Positive test results for DNA antibodies, ribonucleoprotein antibodies and Smith (Sm) antibodies are suggestive of SLE.
Differential diagnosis
- Skin changes due to SLE Systemic Lupus Erythematosus (Sle) (discoid skin lesions, butterfly rash)
- Polymorphous light eruption: recurring, small pruritic papules on the chest and backs of the hands in the spring, appearance directly linked to the time elapsed from sun exposure
- Drug-induced photodermatitis and other photodermatitis Photodermatitis
- Rosacea Rosacea: papules and pustules, telangiectasia, lesions only on the face
- Psoriasis Psoriasis: typical sites of predilection, nail involvement
- Tinea Dermatomycoses: isolated lesions with scaling around the borders
- The treatment of general symptoms follows the guidelines given for SLE Systemic Lupus Erythematosus (Sle).
- Treatment aims to eliminate symptoms, control the active disease, prevent exacerbations, minimise drug adverse effects as well as to improve the quality of life.
- Active skin lesions require effective management in order to prevent scarring of the skin and consequent cosmetic issues.
- Avoidance of the sun's UV radiation by wearing correct clothing and using sun screens may prevent the development of new lesions.
- Less aggressive lesions can be treated with topical therapy.
- An adequately long treatment period with moderately potent to potent glucocorticoid creams, for example once daily in the evening for 2-3 weeks, thereafter twice a week for 1-2 months as required.
- Tacrolimus cream is also a good choice, for example twice daily until the rash has started to subside, thereafter twice a week as required.
- Systemic treatment
- The first-line treatment is hydroxychloroquine. Regular laboratory monitoring is recommended during the treatment (full blood count, ALT) as well as check-ups by an ophthalmologist (before treatment if needed and then every 5 years).
- Oral glucocorticoids may be considered as short term treatment in a severe exacerbation, for example prednisolone 30-40 mg in the mornings whilst tapering the dose down over 2-4 weeks.
- Other treatment alternatives include immunosuppressive medication prescribed under the supervision of a dermatologist or rheumatologist (e.g. methotrexate, azathioprine, mycophenolate mofetil or dapsone, thalidomide or retinoids).
Specialist consultation and monitoring
- The diagnosis and treatment of DLE are the responsibility of a dermatologist.
- In mild disease forms, the monitoring may be carried out in primary health care.
- Treatment response may show great variation, and the disease may reactivate after many years of remission.
- If SLE is suspected, a referral to a specialist in internal medicine or a rheumatologist is required.