NB-UVB 311 nm in Nonsegmental Vitiligo: Cohort Outcomes, Protocols, and Safety (n≈150–200)

Key Takeaways

Backbone therapy for generalized/nonsegmental vitiligo with best responses on face/neck; acral lesions remain hardest.
Typical schedules: 2–3×/week, incremental dosing from MED-based start; visible perifollicular islands at 6–10 weeks, peak gains by 24–36 weeks.
Combination with tacrolimus/pimecrolimus or excimer for focal areas improves speed and magnitude of response.
Safety: mostly grade 1–2 erythema/dryness; careful dose-holding prevents burns. Eye/thyroid shielding per protocol.

Abstract

We summarize cohort data (n≈150–200 across centers) for NB-UVB 311 nm in nonsegmental vitiligo, focusing on practical protocols, anatomic response heterogeneity, time-to-repigmentation, maintenance strategies, and adverse events. Structured tables below are prepared for insertion of site-specific numerics (F-VASI/T-VASI, responder thresholds).

Protocols & Dosing

Table 1. Common NB-UVB schedules.

Parameter	Typical setting	Notes
Frequency	2–3 sessions/week	Minimum 48h between sessions
Start dose	70% MED or 200–300 mJ/cm²	Phototype-adjusted
Increment	10–20% per session	Hold/reduce if erythema >24h
Course length	24–36 weeks initial	Extend to 9–12 months if improving
Protection	Goggles; genital/thyroid shielding	Remove sunscreen from treated areas

Efficacy by Anatomic Zone

Table 2. Typical response patterns.

Zone	Response	Notes
Face/neck	Highest (F-VASI responders common)	Early perifollicular islands
Trunk/non-acral limbs	Moderate	Slower than face
Acral (hands/feet)	Low	Add excimer or surgery when stable

Time Course & Durability

First visible islands: 6–10 weeks; plateau often after 24–36 weeks.
Maintenance: taper to weekly→biweekly for 2–3 months to reduce relapse risk, especially on face/neck.

Combination Strategies

Tacrolimus 0.1% on face/neck between sessions improves speed and magnitude.
Pimecrolimus 1% for steroid-sparing on periorificial areas.
Excimer 308 nm for focal, resistant edges or acral zones.
Consider topical JAK for facial persistence after adequate NB-UVB exposure.

Safety

Table 3. Adverse events (typical cohort frequencies).

Event	Pattern	Management
Erythema/dryness	Mild, dose-related	Hold dose; emollients
Pruritus	Occasional	Moisturizers; antihistamines prn
Burns	Rare with protocolized increments	Immediate dose reduction/hold

Outcome Tables (framework)

Table 4. Efficacy outcomes (fill with study numerics).

Outcome	NB-UVB cohort	Interpretation
F-VASI % change (week 24)	—	Primary facial endpoint
T-VASI % change (week 24–36)	—	Total body response
F-VASI50/75 responders	—	Responder thresholds
Relapse at 6–12 mo	—	Need for maintenance

Limitations

Retrospective bias, heterogeneous dosing and endpoints across centers, limited long-term off-therapy durability data, and under-reporting of acral outcomes.

References

Multicenter and single-center cohorts (n≈150–200) reporting NB-UVB 311 nm outcomes using VASI-based metrics.
Guidelines on NB-UVB dosing, MED testing, and safety monitoring in vitiligo.
Combination studies with calcineurin inhibitors and excimer therapy.