Systemic lupus erythematosus (SLE) Flashcards

1
Q

Define SLE.

A
  • SLE is a chronic autoimmune multisystem disorder
  • of unknown aetiology
  • characterised by the presence of ANA
  • it most frequently involves the skin and joints
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2
Q

What criteria is used to diagnose SLE?

A

2019 EULAR/ACR classification system

Entry criterion = Antinuclear antibodies (ANA) at a titre of ≥1:80 on HEp-2 cells or an equivalent positive test (ever)

If absent, do not classify as SLE; if present, apply additive criteria: These do not need to occur simultaneously and only need to occur once. Only count highest in each domain. SLE classification requires at least one clinical criterion and ≥10 points:

Clinical domains and criteria

  • Constitutional
    • Fever, 2 points
  • Haematological
    • Leukopenia, 3 points
    • Thrombocytopenia, 4 points
    • Autoimmune haemolysis, 4 points
  • Neuropsychiatric
    • Delirium, 2 points
    • Psychosis, 3 points
    • Seizure, 5 points
  • Mucocutaneous
    • Non-scarring alopecia, 2 points
    • Oral ulcers, 2 points
    • Subacute cutaneous OR discoid lupus, 4 points
    • Acute cutaneous lupus, 6 points
  • Serosal
    • Pleural or pericardial effusion, 5 points
    • Acute pericarditis, 6 points
  • Musculoskeletal
    • Joint involvement, 6 points
  • Renal
    • Proteinuria >0.5 g/24 hours, 4 points
    • Renal biopsy class II or V lupus nephritis, 8 points
    • Renal biopsy class III or IV lupus nephritis, 10 points

Immunology domains and criteria

  • Antiphospholipid antibodies
    • Anticardiolipin antibodies OR anti-beta2-glycoprotein 1 antibodies OR lupus anticoagulant, 2 points
  • Complement proteins
    • Low C3 OR low C4, 3 points
    • Low C3 AND low C4, 4 points
  • SLE-specific antibodies
    • Anti-double-stranded (ds)DNA antibody OR anti-Smith antibody, 6 points
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3
Q

What is the epidemiology of SLE?

A
  • F>M
  • Peaks at 30-70yo
  • Increasing incidence
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4
Q

What are the aetiological factors for SLE?

A

Genetics

Drugs - commonly procainamide, minocycline, terbinafine, sulfasalazine, isoniazid, phenytoin, and carbamazepine

Infectious agents - EBV, PVB19, CMV, HIV1

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5
Q

What is the pathophysiology of SLE?

A

Failure of immune tolerance to your own antigens during rapid clearance of cells through apoptosis

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6
Q

What antibodies are associated with SLE? Which are most specific?

A
  • ANA
  • anti-dsDNA - very specific
  • anti-Sm - most specific
  • ati-histone - associated with drug induced SLE
  • antiphospholipid antibodies
  • anti-Ro

anti-Sm are part of the ENA panel

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7
Q

What are anti-RNP antibodies characteristic of?

A

Mixed connective tissue disease

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8
Q

What investigations would you do for diagnosis of SLE?

A

Bedside/bloods:

  • Urinalysis - haematuria, casts or proteinuria (PCR/ACR)
  • ANA, anti-dsDNA, anti-Sm, antiphospholipid antibodies
  • FBC -anaemia, leukopenia, thrombocytopenia; rarely pancytopenia
  • U&Es - elevated urea and creatinine
  • aPTT - may be prolonged in presence of antiphospholipid antibodies
  • ESR and CRP

Imaging:

  • ECG - exclude other causes of chest pain
  • CXR - pleural effusion, infiltrates, cardiomegaly

Other (not necessary for diagnosis):

  • Renal biopsy/USS
  • Complement levels
  • Pulmonary function tests
  • Brain MRI
  • Echo
  • Skin biopsy
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9
Q

What are the signs and symptoms of SLE?

A
  • Malar rash
  • Photosensitive rash
  • Discoid rash
  • Fatigue
  • Weight loss
  • Fever
  • Oral ulcers
  • Alopecia
  • Arthralgia/arthritis - usually of large joints
  • Fibromyalgia
  • Raynaud’s phenomenon
  • Chest pain and SOB
  • V/A thrombosis
  • HTN
  • Nephrosis (e.g. oedema signs)
  • Lymphadenopathy
  • Abdo pain, vomiting or diarrhoea
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10
Q

What HLA are associated with SLE?

A

HLA-B8

HLA-DR2

HLA-DR3

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11
Q

What type of endocarditis occurs in patients with SLE?

A

Libman-Sacks endocarditis

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12
Q

What is shown?

A

SLE malar rash

a) Photograph of a face with skin rashes sparing the bridge of the nose and malar area. b) Photograph of a face showing asymmetric hyperpigmented, polycylic, and annular scaly plaques with scaling involving pre-auricular area and cheek

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13
Q

What are the dermatological features of SLE?

A
  • Acute:
    • Malar rash - spares nasolabial folds, hyperkeratosis will be seen on darker skin
    • TEN-like rash
    • Generalised rash
    • May look like ringworm
  • Subacute
    • Anuular
    • Papulo-squamous
    • Drug-induced
    • Rowell syndrome
  • Chronic
    • Lupus panniculitis
    • Discoid lupus

Other

  • Oral ulcers
  • Non-scarring alopecia (diffuse thinning or hair fragility with visible broken hairs)
  • Raynaud’s phenomenon

Fatigue, fever, weight loss

Lymphadenopathy

Synovitis involving two or more joints, characterised by swelling or effusion OR tenderness in two or more joints and 30 minutes or more of morning stiffness

Serositis

Pleuritis

Pleural effusions

ILD

pulmonary hypertension

Cardiovascular

pericarditis

Myocarditis

endocarditis

arterial and venous thrombosis

premature atherosclerosis

Renal

Lupus nephritis

Neurological

Seizures

Cranial nerve abnormalities

Psychosis

Fibromyalgia

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14
Q

What are the cardiovascular and pulmonary features of SLE?

A

Cardiovascular:

  • Pericarditis
  • Myocarditis - may present with tachycardia, arhythmias, conduction defects, unexplained cardiomegaly
  • Endocarditis - Libman-Sacks non-bacterial
  • Arterial and venous thrombosis
  • Premature atherosclerosis

Pulmonary:

  • Pleuritis
  • Pleural effusions
  • Interstitial lung disease
  • Pulmonary hypertension (echo for this)
  • PE
  • Shrinking lung syndrome
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15
Q

What are the features of joint involvement in SLE?

A
  • Symmetrical
  • Peripheral
  • Pain worse in mornings and associated with stiffness
  • Deformity e.g. correctable ulnar deviation and joint subluxations
  • No damage to joints i.e. no radiographical damage
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16
Q

How high is cardiovascular risk in SLE compared to normal population?

A

x2-3 - therefore GPs are asked to monitor using QRISK2 score to reduce this

17
Q

What are the CNS/neuropsychiatric features of SLE?

A
  • Seizures
  • CN abnormalities
  • Psychosis
  • Depression
  • Encephalopathy
18
Q

What are the features of renal involvement in SLE?

A
  • Lupus nephritis - 10% with this will get end-stage renal failure eventually
  • HTN
  • Nephrotic syndrome
  • Renal failure
19
Q

What are the GIT features of SLE?

A
  • Oral ulcers
  • Dysphagia due to oesophageal hypomobility
  • Abdominal pain - may be due to lupus peritonitis
  • Vomiting
  • Diarrhoea

Pancreatitis in SLE more likely due to azathioprine.

20
Q

Whcih investigations are used for monitoring disease activity in SLE? What questionnaire is used?

A

Physical examination

Bloods:

  • ESR
  • Complement - C4 decreases first, then C3
  • Anti-dsDNA
  • WCC
  • Plt

Other:

  • Spirometry - 6 -12 monthly depending on disease
  • Spot urine for PCR
  • Urinalysis
  • Echo - for pulmonary hypertension

SLEDAI score (below) - 5 or less is remission

21
Q

Which 3 investigations indicate an increase in disease activity in SLE?

A
  • Increasing ESR (CRP is generally less useful in SLE)
  • Falling C4 complement
  • Rising dsDNA
22
Q

What can be used for mucocutaneous problems in SLE?

A
  • Sunscreen
  • Chlorhexidine mouth washes
  • Lidocaine ointment - for oral ulcers
  • Artifical saliva - for dry mouth
  • Hypromellose eye drops - for dry eyes
  • Topical agents (e.g., corticosteroids, calcineurin inhibitors)

etc

23
Q

What is the management of SLE?

A

Conservative

  • Sun protection
  • Smoking cessation - associated with active disease and reduces the therapeutic effect of hydroxychloroquine

Medical:

  • NSAIDs - first line, but avoid in HTN
  • cDMARDS
    • Hydroxychloroquine - recommended for all, ophthalmological screening needed
    • Methotrexate
    • Azathioprine
  • bDMARDS e.g. Biological agents - e.g. belimumab and rituximab
  • Corticosteroids - may be needed long term
24
Q

Is hydroxychloroquine safe in pregnnacy?

A

Yes - can be continued throughout

25
Q

Which cDMARD can cause fertility problems?

A

Cyclophosphamide

26
Q

What is Rowell syndrome?

A

Rare disease consisting of erythema multiforme-like lesions associated with lupus erythematosus. It is a chronic cutaneous manifestation of SLE. Only 96 cases reported.

In contrast to erythema multiforme, the lesions are not in acral or mucosal areas.

27
Q

What is shown?

A

Lupus profundus/lupus panniculitis

  • Can develop at any site
  • Present as persistent, firm, deep, tender nodules
  • Resolve to leave dents in the skin due to atrophy of the fat.