Scleroderma | Figure 3.35
A: Morphea
(Courtesy of Dr. Paul Getz)
B: Morphea
(Courtesy of Dr. Sophie M.
Worobec)
C: Morphea |
| Figure 3.36
A: Systemic sclerosis*
B: Systemic sclerosis*
C: Systemic sclerosis*
*Courtesy of Dr. Paul Getz |
- Morphea (localized scleroderma) (Figure 3.35A–C)
- Localized form of scleroderma with unknown etiology, possibly due to trauma or infection (i.e. Borrelia burgdorferi)
- Presents initially with expanding erythema → turns into ivory-colored sclerotic plaque → eventually softens; typically becomes inactive within 3–5 years
- Variants: disseminated morphea, guttate morphea, linear morphea (linear scleroderma), nodular morphea, morphea profunda, progressive hemifacial atrophy (Parry Romberg syndrome)
- Histology: dense lymphocytic infiltrate around superficial/deep vessels with few eosinophils, inflammation between dermal-subcutaneous fat junction; advanced lesions with dermal sclerosis
- Labs: ± ANA in disseminated or linear morphea (unlikely to see with plaque-type morphea)
- Treatment: topical mid to high potency corticosteroid, topical vitamin D analogue, PUVA or UVA1
- Systemic Sclerosis (SSc) (Figure 3.36A–C)
- Systemic disorder affecting the skin, blood vessels and internal organs; early events in pathogenesis include vascular dysfunction and endothelial injury; fibrosis related to TGF-β, endothelin-1, PDGF, and connective tissue growth factor (CTGF)
- Onset typically in women (30–50 years/old); African American patients with earlier onset and ↑ risk of diffuse disease
- Presents with varying symptoms:
- Cutaneous: pruritus, initial edematous phase (pitting edema of digits) with subsequent sclerosis (shiny, taut appearance) and digital ulcerations, sclerosis may affect arms, face (mask-like) and/or neck; dyspigmentation with leukoderma sparing perifollicular skin (‘salt/ pepper’ sign) or diffuse hyperpigmentation; calcinosis cutis
- Vascular: Raynaud’s phenomenon (vasospasm of digital arteries secondary to cold stimulus with classic color change: white → blue → red)
- Other: symmetric synovitis, migratory polyarthritis, pulmonary (interstitial lung disease → pulmonary fibrosis), cardiac, renal, GI (reflux, dysphagia)
- Labs: ANA (nucleolar/centromeric), anti-Scl-70, anti-fibrillarin, anti-centromere, anti-RNA polymerase
- Histology: normal to atrophic epidermis, hyalinized dermis with ↑ collagen deposition, ↓ adnexal structures, loss of subcutaneous fat
- Treatment:
- Raynaud’s: cold temperature avoidance, calcium channel blockers (nifedipine), low dose aspirin, prostaglandin E1
- Cutaneous ulcers: oral endothelin receptor antagonist (i.e. bosentan) may prevent new ulcers
- Systemic: prostaglandins (prostacyclin), immunosuppressants, D-penicillamine, ACEI
| | | | | | Systemic sclerosis: ↑ expression of extracellular matrix (ECM) proteins from dermal fibroblasts and ↑ deposition of collagen type III | | | | | |
|
- CREST (limited SSc) (Figure 3.37A)
- Limited form of systemic sclerosis
- CREST: calcinosis, Raynaud’s phenomenon, esophageal involvement, sclerodactyly, telangiectasias
- Associated with anti-centromere antibodies, rarely progresses to SSc, better prognosis than SSc
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