Rheumatoid arthritis
Systemic Sclerosis (Scleroderma) Overview for Medical Students | Rheumatology Masterclass Module 1
MODULE 1 · OVERVIEW

Systemic Sclerosis (Scleroderma): Overview & Learning Objectives

A world-class, guideline-referenced introduction to the most lethal autoimmune rheumatic disease — built for medical students preparing for clinical clerkships, USMLE/PLAB, and real-world scleroderma clinics.

1.1 High-Yield Clinical Significance

Systemic sclerosis (SSc), historically called scleroderma, is an orphan autoimmune connective tissue disease characterized by three intertwined pathologic processes acting on virtually every organ system: microvascular injury (vasculopathy), autoimmunity/inflammation, and progressive fibrosis of the skin and internal organs. [Harrison’s, Ch. 360] Although the name “scleroderma” evokes skin thickening, the term SSc is preferred because visceral, not cutaneous, involvement drives prognosis. [EULAR 2023]

Why this matters on the wards and on exams: SSc carries the highest mortality of any autoimmune rheumatic disease — roughly half of affected people eventually die as a direct result of the disease or a related complication. [BSR 2024] The two leading causes of SSc-related death are interstitial lung disease (ILD) and pulmonary arterial hypertension (PAH), together accounting for the majority of SSc mortality. [BSR 2024]

Key epidemiologic facts

  • Estimated incidence: 9–46 new cases per million per year; prevalence in the U.S. approaches 100,000 cases, although true prevalence is likely underestimated because a substantial proportion of patients do not fulfil formal classification criteria. [Harrison’s, Ch. 360] In the UK, roughly 1,000 new cases are diagnosed per year. [BSR 2024]
  • Female predominance of about 4.6:1, most pronounced during the childbearing years and declining after menopause — pregnancy and first-degree family history of SSc each independently raise disease risk (up to 13-fold for a first-degree relative). [Harrison’s, Ch. 360]
  • Race/ethnicity: Black patients have higher age-specific incidence and mortality, more frequently develop diffuse cutaneous disease and ILD, tend to have earlier disease onset, and generally have a worse prognosis. [Harrison’s, Ch. 360]
  • Juvenile-onset SSc (jSSc), defined as onset of the first non-Raynaud manifestation before age 18, is exceedingly rare (prevalence ~3 per 1,000,000) but carries important differences from adult disease, including more frequent overlap features. [BSR 2024]
  • Around 1 in 3 people with SSc develop ILD and 1 in 10 develop pulmonary hypertension — together the leading direct causes of SSc-related death. 1 in 5 develop an overlap connective tissue disease requiring parallel management. [BSR 2024]

The disease at a glance: two major clinical subsets

FeatureLimited Cutaneous SSc (lcSSc)Diffuse Cutaneous SSc (dcSSc)
Skin involvementIndolent onset; limited to fingers, distal to elbows/knees, face; slow progressionRapid onset; extremities, trunk; rapid progression
Raynaud’s phenomenonAntedates skin involvement, sometimes by yearsOnset coincident with or shortly before skin involvement
Interstitial lung diseaseSlowly progressive, generally mildFrequent, early onset, can progress and be severe
Scleroderma renal crisisVery rareOccurs in ~5% (early, <4 years disease duration)
Characteristic autoantibodyAnti-centromereAnti-topoisomerase I (Scl-70), anti-RNA polymerase III

Adapted from Harrison’s Table 360-3 and Table 360-4.

A minority of patients present with the hallmark serologic and vascular features of SSc (Raynaud’s phenomenon, SSc-specific autoantibodies) yet lack cutaneous sclerosis — a benign disease subset termed SSc sine scleroderma. [Harrison’s, Ch. 360]

1.2 Learning Objectives (Mapped to Bloom’s Taxonomy)

1. Remember — Define systemic sclerosis, list its major clinical subsets (dcSSc, lcSSc, SSc sine scleroderma, overlap SSc), and recall the epidemiologic profile including sex, race, and mortality data. Knowledge
2. Understand — Explain the pathogenic triad of vasculopathy, autoimmunity, and fibrosis, and describe how genetic susceptibility (HLA and non-HLA loci) interacts with environmental exposures to trigger disease in a susceptible host. Comprehension
3. Apply — Given a clinical vignette featuring Raynaud’s phenomenon, puffy fingers, and an abnormal nailfold capillary pattern, apply the 2013 ACR/EULAR classification criteria to determine whether a patient meets criteria for SSc. Application
4. Analyze — Differentiate the clinical trajectory, organ-risk profile, and serologic associations of diffuse versus limited cutaneous SSc, and correlate specific SSc-associated autoantibodies (anti-Scl-70, anti-centromere, anti-RNA polymerase III) with distinct patterns of organ involvement. Analysis
5. Evaluate — Critically appraise current BSR (2024) and EULAR (2023) guideline recommendations for organ-based screening and treatment, and justify a risk-stratified, multidisciplinary approach to management of a newly diagnosed patient with early diffuse cutaneous SSc. Evaluation

1.3 How This Module Fits Into the Course

This overview is Module 1 of a 13-module systemic sclerosis curriculum. Each subsequent module builds toward full clinical competency — from molecular pathogenesis, through pattern recognition on imaging, to guideline-concordant management and USMLE/PLAB-style mastery testing. Bookmark this page as your anchor: every later module will refer back to the subsets, epidemiology, and objectives defined here.

Educational content for medical trainees. Synthesized from Harrison’s Principles of Internal Medicine (Ch. 360), the 2024 BSR Guideline for Management of Systemic Sclerosis (Rheumatology 2024;63:2956–2975), the 2023 EULAR Recommendations for the Treatment of Systemic Sclerosis (Ann Rheum Dis 2024), and the 2013 ACR/EULAR Classification Criteria for Systemic Sclerosis (Arthritis Rheum 2013;65:2737–2747). Not a substitute for institutional curricula or clinical judgment.

Coming Up Next — Module 2

Pathogenesis of Systemic Sclerosis: Now that you understand what SSc is, Module 2 explains why it happens. You’ll walk through the disease “as a story” — from HLA and non-HLA genetic susceptibility loci, through environmental and occupational triggers (silica, solvents, viral infections), to the three synchronous pathomechanistic processes of microangiopathy, immune dysregulation, and fibrosis that converge to produce the clinical phenotype of SSc.

Continue to Module 2: Pathogenesis →
Module 1 of 13 complete