Cutaneous Squamous Cell Carcinoma (cSCC)

Cutaneous squamous cell carcinoma arises from keratinocytes due to cumulative UV damage and other carcinogens. It ranges from low-risk lesions curable with excision to high-risk tumors with metastatic potential, especially in immunosuppressed patients. Variants include in situ SCC (Bowen disease), keratoacanthoma-type, and invasive cSCC with diverse histologies. Accurate risk stratification (tumor size, depth, differentiation, location, perineural invasion, host factors) guides management and surveillance.

Epidemiology and Risk Factors

• Second most common skin cancer; incidence rising.
• Risks: chronic UV, fair skin, older age, actinic keratoses/field damage, immunosuppression (solid organ transplant recipients have 65–250× risk), radiation scars/burns, HPV (periungual/genital), arsenic, chronic wounds.
• In skin of color, cSCC often arises in scars, ulcers, or areas of inflammation; later presentation and worse outcomes.

Clinical Features

• Hyperkeratotic papule/plaque or nodule with scale/crust; can ulcerate or be tender.
• cSCC in situ (Bowen): well-demarcated erythematous scaly patch/plaque.
• Keratoacanthoma-type: rapid-growing crateriform nodule with keratin plug; many behave as low-grade SCC but treat as SCC.
• High-risk sites: ear, lip, central face, hands, genitalia; tumors on scars/chronic ulcers (Marjolin).

Diagnosis and Staging

• Biopsy: shave or punch to confirm SCC and assess differentiation.
• High-risk features: thickness >2 mm or Clark IV/V, poor differentiation, perineural invasion, ear/lip location, size thresholds (e.g., >2 cm trunk/extremities; lower thresholds on face), immunosuppression.
• Staging: AJCC 8th (head/neck) and BWH staging systems incorporate size, depth, and perineural invasion; useful for nodal risk.
• Imaging: ultrasound/CT/MRI for high-risk tumors to assess nodes or perineural spread.

Management

1. Surgical

• Standard excision with 4–6 mm margins for low-risk cSCC; wider for high-risk.
• Mohs micrographic surgery for high-risk locations, recurrent tumors, poorly defined borders, perineural involvement.
• Sentinel lymph node biopsy: consider in select very high-risk cases; evidence evolving.

2. Destructive/field treatments

• cSCC in situ: C&E, cryosurgery, topical 5-FU or imiquimod, or PDT on non–hair-bearing skin; surgery preferred for hair-bearing or thick lesions.
• Invasive cSCC: destructive methods generally avoided unless low-risk and superficial.

3. Radiation therapy

• Primary treatment for nonsurgical candidates; adjuvant for positive margins, extensive perineural invasion, or nodal disease.

4. Systemic/advanced disease

• PD-1 inhibitor cemiplimab (first-line) and pembrolizumab for unresectable/metastatic cSCC; high response rates and durability.
• EGFR inhibitors (cetuximab) when immunotherapy unsuitable.
• Multidisciplinary management for nodal or advanced disease (surgery + adjuvant RT ± systemic).

5. Special populations

• Solid organ transplant recipients: reduce immunosuppression if feasible (switch to mTOR inhibitors), intensive surveillance, field therapy, and chemoprevention (acitretin).
• Periungual/anogenital SCC: evaluate for HPV; margin-controlled surgery.

6. Follow-up and Prevention

• Regular skin and nodal exams (every 3–6 months initially for high-risk).
• Treat field cancerization; sun protection; nicotinamide 500 mg bid may reduce NMSC burden.
• Educate on self-exams and early signs.

References (recent guidelines and key reviews)

• NCCN/AAD guidelines for cSCC, 2022–2024.
• AJCC/BWH risk stratification and outcomes studies, 2021–2024.
• Immunotherapy in advanced cSCC trials and real-world data, 2021–2024.