Ocular surfaceMucosal SCCICD-10 C69.0

Ocular surface squamous neoplasia (OSSN)

OSSN; conjunctival intraepithelial neoplasia (CIN); corneal-conjunctival intraepithelial neoplasia; conjunctival SCC; squamous cell carcinoma of the conjunctiva

Ocular surface squamous neoplasia is a spectrum of squamous proliferations of the conjunctiva and cornea — from mild dysplasia and carcinoma in situ (collectively CIN, conjunctival intraepithelial neoplasia) through to invasive squamous cell carcinoma. UV is the dominant risk factor; HIV and HPV are recognised co-factors, with substantially elevated incidence in sub-Saharan Africa. Clinically OSSN presents as a gelatinous, leukoplakic or papilliform plaque at the limbus or interpalpebral conjunctiva with feeder vessels. UK management combines topical chemotherapy (mitomycin C, interferon α-2b) with surgical excision using a no-touch technique and adjunctive cryotherapy. Specialist ocular oncology service involvement is essential for invasive disease.

CurrentLast reviewed 15 May 2026

Clinical features

  • Gelatinous, leukoplakic or papilliform conjunctival mass at the limbus or interpalpebral conjunctiva — usually unilateral.
  • Prominent feeder vessels and surface vascular hairpin loops.
  • Corneal involvement appears as a translucent grey opacification with whorl-like patterns.
  • Median age 60–70 in temperate climates; younger (~ 40–50) in equatorial regions and in HIV-positive individuals.
  • Male predominance overall.

Risk factors

  • Chronic UV exposure — the dominant risk factor; outdoor occupations, equatorial latitudes.
  • HIV — substantial relative-risk elevation; OSSN is an AIDS-defining illness in some classifications.
  • HPV — particularly HPV-16; co-factor; relevance debated.
  • Xeroderma pigmentosum.
  • Atopic / chronic ocular surface inflammation.
  • Cigarette smoking.

Imaging and diagnosis

  • Slit-lamp examination with rose-bengal or lissamine green staining — neoplastic epithelium retains stain.
  • Anterior segment optical coherence tomography (AS-OCT) — highly characteristic abrupt transition from normal thin epithelium to thickened hyper-reflective neoplastic epithelium.
  • Ultrasound biomicroscopy (UBM) — for deeper invasion / scleral involvement.
  • Impression cytology or incisional biopsy for histological diagnosis (often after empirical topical therapy in obvious cases).

Management

  • Topical chemotherapy first-line in most UK practice:
    • Mitomycin C 0.02–0.04% drops, 4 × daily for 7 days, then 7-day rest, for 3–6 cycles.
    • Interferon α-2b 1 million IU/mL drops, 4 × daily for 3–6 months.
    • 5-fluorouracil 1% drops, 4 × daily for 4-day cycles, repeated.
  • Topical therapy avoids surgical excision in many cases and is well-tolerated; the principal toxicity is conjunctival inflammation and toxic keratopathy.
  • Surgical excision for tumours unresponsive to topical, large tumours, or those with invasive features:
    • "No-touch" technique to avoid tumour seeding.
    • 4 mm clear margins.
    • Adjunctive double freeze-thaw cryotherapy to conjunctival edges.
    • Amniotic membrane graft for large defects.
  • Brachytherapy (Sr-90 or Ru-106) for residual disease, recurrent disease or scleral invasion.
  • Orbital enucleation / exenteration — for advanced OSSN with deep scleral or orbital invasion.
  • Concurrent assessment / treatment of HIV.
  • Photoprotection — UV-blocking sunglasses, hat.

Prognosis

  • Excellent prognosis for CIN / in situ disease — recurrence after appropriate treatment 5–10%.
  • Invasive disease has higher recurrence; rarely regional or distant metastasis.
  • Lifelong surveillance — 3-monthly for 1–2 years, then 6-monthly.

References

  1. Shields JA, Shields CL. Intraocular Tumors — Atlas and Textbook. Wolters Kluwer; 2016.
  2. Kim BH, Kim MK, Wee WR. Topical mitomycin C in ocular surface squamous neoplasia — meta-analysis. Cornea; 2016.
  3. Stuart KV et al. Ocular surface squamous neoplasia — incidence, management, prognosis. Br J Ophthalmol; 2020.

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