FindTrial
Sign In

Effect Of Topical Prostaglandin F2α Analogs,Fractional CO2 Laser, Excimer Laser Or Their Combination In Treatment Of Vitiligo

Safety And Efficacy Of Topical Prostaglandin F2α Analogs In Combination With Fractional CO2 Laser And 308 Excimer Light In Treatment Of Vitiligo

Status
UNKNOWN
Phases
Phase 4
Study type
Interventional
Source
ClinicalTrials.gov
Registry ID
NCT04577027
Enrollment
30
Registered
2020-10-06
Start date
2021-01-01
Completion date
2022-04-01
Last updated
2020-10-22

For informational purposes only — not medical advice. Sourced from public registries and may not reflect the latest updates. Terms

Conditions

Vitiligo, Excimer Laser, Fractional CO2 Laser

Brief summary

Vitiligo is a chronic disease with an unpredictable clinical course, characterized by the appearance of white macules and patches on the skin and mucous membranes due to the disappearance of melanocytes in the affected area. It affects approximately 0.5% - 2% of the population worldwide and may occur at any age. Vitiligo is caused by a dynamic interplay between genetic and environmental risks that initiates an autoimmune attack on melanocytes in the skin.

Detailed description

The treatment of vitiligo has been a challenge for dermatologists. Recent reports have highlighted darkening of iris, and eyelashes and periocular hyperpigmentation induced by prostaglandin F2α analogues used for the treatment of glaucoma (as travoprost). Extrapolating these findings in the treatment of vitiligo. The beneficial effect of fractional CO2 laser on vitiligo is postulated to come from the release of cytokines and growth factors that act as mitogens for melanogenesis . The preceding laser also alters the skin barrier, which results in increased penetration of topical drugs and ultraviolet (UV) radiation. 308 nm excimer laser is a monochromatic, target type treatment and allows the delivery of higher fluences to the lesions and avoids damage to the surrounding normal skin resulting in a faster and more effective pigmentation with minimal side effects.

Interventions

DRUGTopical travoprost 0.004% solution

30 Patches treated with Topical Travoprost 0.004% solution: Topical travoprost 0.004% solution once daily (1 drop for each 2.5 x 2.5 cm2) for 3 months.

DEVICEFractional CO2 laser

30 Patches treated with Fractional CO2 laser: Fractional CO2 laser sessions twice monthly for 3 months, parameters settings as follows: Energy\\ dot 100mj, pulse duration 5ms, density level 17, pattern: array, depth level 1, 2 passes used

DEVICEExcimer laser

30 Patches treated with Excimer laser: Excimer laser sessions will be repeated twice weekly on the selected patch only, The starting dose will be 200 mj /cm2, an increase of 100 mJ/cm2 in the following session if no erythema appears, an increase of 50 mJ/cm2 every session till the appearance of erythema that lasts 24 hours or more.

OTHERCombination therapy

30 Patches treated with Combination therapy: Fractional CO2 laser twice per month followed by application of topical travoprost 0,004% daily and excimer laser twice weekly .

OTHERExcimer laser and travoprost

30 Patches treated with Excimer laser twice weekly and topical travoprost once daily for 3 months

OTHERfractional CO2 laser and topical travoprost

30 Patches treated with fractional CO2 laser twice monthly and topical travoprost once daily for 3 months

Sponsors

Assiut University
Lead SponsorOTHER

Study design

Allocation
NA
Intervention model
SINGLE_GROUP
Primary purpose
TREATMENT
Masking
NONE

Masking description

no masking

Eligibility

Sex/Gender
ALL
Age
12 Years to 60 Years
Healthy volunteers
No

Inclusion criteria

1. Patients older than 12 years. 2. Patients with generalized non-segmental vitiligo. 3. No previous treatment for vitiligo in the last 1 month. 4. Patients who were unresponsive to medical treatment or photo therapy for at least 3 months.

Exclusion criteria

1. Patients with sensitivity to travoprost. 2. Patients with photosensitivity. 3. Patients with history or active skin cancer. 4. No other dermatological or systemic diseases. 5. Active infections . 6. Pregnant or lactating females.

Design outcomes

Primary

MeasureTime frameDescription
clinical improvement through VASI score9 monthsVASI score will be calculated for each patient at start, every 4 weeks and 6 months after the last session. VASI = ∑ all treated sites \[number of hand units\] X \[% residual depigmentation\].

Secondary

MeasureTime frameDescription
Patients satisfaction9 monthsaccording to the following scale: 1. dissatisfied 2. neutral 3. somewhat satisfied 4. moderately satisfied 5. very satisfied
percent of repigmentation9 monthsThe percent of repigmentation will be calculated every 4 weeks of treatment and 6 months after the last session by a scoring system . \< 25% repigmentation (poor response). 25-50% repigmentation (fair response). 50-75% repigmentation (good response). \> 75% repigmentation (excellent response).
Histopathological evaluation9 monthsSkin biopsy will be taken from the treated lesions after treatment, Hematoxylin and eosin-stained slides will be examined microscopically to evaluate the epidermal and dermal pathological changes: (1) evaluation of dermal perivascular inflammatory infiltrate density; (2) signs of pigmentation in the form of residual melanin in epidermis or dermal melanophages .

Contacts

Primary ContactHatem Zidan, Prof.DR
hzma03@yahoo.com01003420217
Backup ContactYasmin Tawfik, DR

Outcome results

None listed

Source: ClinicalTrials.gov · Data processed: Feb 4, 2026