NB-UVB 311 nm for Vitiligo: Cohort Evidence, Protocols, Predictors, and Safety

Key Takeaways

  • NB-UVB (311–313 nm) consistently induces clinically meaningful repigmentation across multiple cohorts; face responds best, acral sites worst.
  • Typical regimens are 2–3 sessions/week with stepwise dose escalation; early visible response predicts stronger endpoints.
  • Large population data suggest no increase in melanoma or non-melanoma skin cancer risk with long-term NB-UVB in vitiligo; actinic keratoses may rise after very high session counts.
  • Compared with PUVA, NB-UVB offers similar or better effectiveness with fewer adverse effects and simpler logistics.

Abstract

This scholarly review synthesizes outcomes from key NB-UVB (311 nm) cohorts in vitiligo, summarizes practical dosing protocols, highlights predictors of response (anatomic site, early improvement, phototype), and reviews long-term safety including comparative data versus PUVA.

Cohorts & Outcomes

Table 1. Representative NB-UVB cohort studies in vitiligo.
Study Design / n Regimen Primary outcomes Notes
Scherschun et al., 2001 (JAAD) Retrospective; n=7 3×/wk; start 280 mJ/cm²; +15% each session 5/7 achieved >75% repigmentation (mean 19 treatments); others 50% and 40% after 46–48 treatments Mild erythema/pruritus; rapid facial response
Nicolaidou et al., 2007 (JAAD) Prospective; n=70 2×/wk ≥75% repigmentation: face 34.4%; body 7.4%; 14.3% maintained stability 4 years post-therapy Darker phototypes and early responders fared better
Kanwar et al., 2005 (Clin Exp Dermatol) Pediatric; n=26 (20 completed) 3×/wk up to 1 year Marked–complete repigmentation in 15/20 (75%); moderate 20%; mild 5% Safe and effective in children
Hamzavi et al., 2004 (JAAD) Parametric VASI model NB-UVB course Expected mean ≈42.9% repigmentation at 6 months; trunk & non-acral areas respond best Supports use of VASI for quantitative tracking
Westerhof & Nieuweboer-Krobotova, 1997 (Arch Dermatol) Comparative vs topical PUVA 311 nm UV-B vs PUVA NB-UVB efficacy comparable to PUVA with fewer adverse effects Helped establish NB-UVB as first-line option

Dosing Protocols

  • Frequency: 2–3 sessions/week; avoid back-to-back days for sensitive sites.
  • Escalation: Start around 200–300 mJ/cm² (clinic-specific) and increase 10–20% per session aiming for mild, short-lived erythema.
  • Adjustments: Hold/escalation pauses for symptomatic burns; reduce dose for face/intertriginous areas; gradual re-titration after missed weeks.
  • Monitoring: Standardized photos; VASI/F-VASI to quantify change; reassess at ~12–16 weeks for early response.

Predictors of Response

  • Anatomic site: Face > trunk/non-acral > distal acral areas.
  • Early improvement: Visible repigmentation in the first month correlates with stronger endpoints.
  • Phototype: III–V may achieve higher rates of cosmetically acceptable repigmentation on the face.

Safety & Long-Term Data

Population-scale analyses in vitiligo report no increase in melanoma or non-melanoma skin cancer with NB-UVB, even at high cumulative sessions; actinic keratoses may rise after very high exposures. Compared with PUVA, NB-UVB avoids psoralen side effects and complex shielding/logistics.

Limitations

Heterogeneity in dosing schedules, definitions of response, and follow-up complicates cross-study comparisons; acral disease remains refractory and may require adjuncts or surgical approaches.

References

  1. Westerhof W, Nieuweboer-Krobotova L. Treatment of vitiligo with UV-B vs topical PUVA. Arch Dermatol. 1997.
  2. Scherschun L, Kim JJ, Lim HW. Narrow-band UVB is a useful and well-tolerated treatment for vitiligo. J Am Acad Dermatol. 2001.
  3. Hamzavi I, et al. Parametric modeling of NB-UVB using VASI in vitiligo. J Am Acad Dermatol. 2004.
  4. Kanwar AJ, Dogra S. Narrow-band UVB for generalized vitiligo in children. Clin Exp Dermatol. 2005.
  5. Nicolaidou E, et al. Efficacy, predictors, and long-term follow-up with NB-UVB. J Am Acad Dermatol. 2007.
  6. Bae JM, et al. Skin cancer/precancer risk in vitiligo with NB-UVB. JAMA Dermatol. 2020.
  7. Harris JE, Scharf M. Vitiligo nbUVB Treatment Protocol (guideline PDF).
  8. Khanna U. What is new in NB-UVB therapy for vitiligo? Review.

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