Ayurveda is an alternative medicine system heavily practiced in India and Nepal. The doshas, which represent the three physiological energy descriptors, are the primary determinants of health and disease in Ayurveda.²⁸ Ayurvedic medicine encompasses a variety of holistic practices and treatments, many of which are botanically based, and is widely used in the treatment of vitiligo.

Shvitrahara lepa is an Ayurvedic topical ointment that has been utilized in conjunction with an oral decoction known as Shvitrahara kashaya for the treatment of vitiligo. A decoction is an extract prepared via boiling herbal material. The ointment contains Haratala, an arsenic containing compound with immunomodulatory properties, which has been proposed to prevent the self-destruction of melanocytes in patients with vitiligo.²⁹ In 2011, Dhanik et al conducted a randomized, controlled clinical trial to assess the role of Shvitrahara kashaya and Shvitrahara lepa on lesion characteristics in patients with either segmental or generalized vitiligo.²⁹ Three treatment groups were included in the analysis: Group I (n = 25) received both the decoction and ointment, Group II (n = 15) received just the ointment, and Group III (n = 10) received oral psoralens and UVA therapy (PUVA) to serve as a conventional medical standard. Those receiving only topical Shvitrahara lepa (Group II) experienced a mean reduction in vitiliginous lesion body surface area of 0.41 ± 0.28 cm² (p < 0.001). Although this result is statistically significant, the mean reduction in area of vitiliginous lesions in both Group I and Group III were significantly greater than that in Group II. Similarly, although Group II experienced an average decrease in lesion number of 3.27 ± 0.96 (p < 0.001), the mean change in lesion number was significantly greater in both Group I and Group III. There was no significant difference in the reduction in the number of lesions between Group I and III, although Group III subjects experienced a significantly greater reduction of total surface area than both Group I and II.

Eight out of 10 Group III subjects developed sunburn, severe itching, and gastric upset upon taking oral psoralen. The mild improvement in lesion surface area and number among subjects receiving solely topical Shvitrahara lepa suggests that the topical ointment has synergistic effects on lesion characteristics in patients with vitiligo when combined with oral Shvitrahara kashaya. One of the concerns that was not addressed by the authors is the potential for arsenic exposure and toxicity with long-term use, as long-term arsenic exposure is associated with several medical issues such as the development of cutaneous malignancies.

Cucumis melo, also known as muskmelon, is a plant species of the Cucurbitaceae family. Extracts are rich in antioxidants and contain high superoxide dismutase (SOD) activity which help counteract the oxidative stress implicated in melanocyte deconstruction.³⁰ Two studies have assessed the efficacy of a topical gel containing Cucumis melo, SOD, and catalase in the treatment of vitiligo.

Yuksel et al evaluated the change in surface area of vitiligo patients receiving either NB-UVB (n = 15) or NV-UVB with topical Cucumis melo superoxide dismutase and catalase gel (n = 15). However, they found no significant difference in healing percentages of measured areas between each group.³¹ Similarly, a 2012 study assessed the efficacy of the gel alone against a placebo gel and found no significant changes in lesion area and perifollicular pigmentation in both groups.³² Both pilot studies suggest that the combination gel containing Cucumis melo, superoxide dismutase, and catalase is not beneficial or effective in the topical treatment of vitiligo.

A distinct topical formulation containing Cucumis melo extract, acetylcysteine, and phenylalanine was assessed in an open observational study.³³ The study included four treatment groups: Group A was treated with the gel alone, twice daily; Group B was treated with UVB phototherapy alone, once weekly; Group C was treated with twice-daily topical gel and once weekly UVB phototherapy; Group D was treated with clobetasol propionate 0.05% ointment, a class 1 topical corticosteroid, twice daily. Greater than 75% repigmentation was observed in 38.4% of Group A subjects, 61.1% of Group B subjects, 73.5% of Group C subjects, and 56.2% of Group D subjects. Less than 10% of subjects in each group depicted less than 25% repigmentation. The results depict the moderate efficacy of topical Cucumis melo extract, acetylcysteine, and phenylalanine formulation. Furthermore, the results of Groups A-C depict the potential for the formulation to have a synergistic effect when combined with phototherapy. It was noted that calcineurin inhibitors were not included in the comparison. Furthermore, it is interesting that phototherapy was delivered only once a week when typical regimens are set at two or three times a week. In addition, it is important to note that phenylalanine is a precursor in melanogenesis; phenylalanine hydroxylation produces tyrosine, which further derives melanin. As such, it is difficult to conclude the efficacy of Cucumis melo extract alone based on the gel’s incorporation of phenylalanine but only in combination with phenylalanine and acetylcysteine.

Curcumin, a polyphenol derived from the golden spice turmeric (Curcuma longa), has been used for the treatment of various diseases due to its antioxidant, anti-proliferative, anti-inflammatory, antiviral, antibacterial, and antifungal properties.³⁰ In 2010, Asawanonda and Klahan assessed the efficacy of a topical tetrahydrocurcuminoid cream in combination with NB-UVB phototherapy (Group A) versus NB-UVB phototherapy alone (Group B) in the treatment of vitiligo.³⁴ Scored according to a nine-point scale, both treatment groups exhibited statistically significant degrees of repigmentation from baseline; at 12 weeks, Group A experienced a score increase of 1.9 ± 1.37 (p = 0.001) and Group B experienced a score increase of 1.7 ± 0.1 (p = 0.006). Although the group receiving tetrahydrocurcuminoid cream exhibited slightly better repigmentation, the difference between the groups was not statistically significant. However, this pilot study only included ten subjects, and further analysis with a larger study population is necessary to assess the efficacy of topical tetrahydrocurcuminoid cream in the treatment of vitiligo.

A randomized clinical trial assessed the efficacy of Vitilinex, a topical formulation containing herbal bio-actives, on the repigmentation among 62 patients with vitiligo.³⁵ Vitilinex was composed of two products. The first was a Skin Prep lotion (containing Centipeda cunninghamii, Aloe vera, terpinol-4-ol and dihydro avenanthramide D) and an emollient (containing black cumin seed oil, black pepper coleus forskohlii, Psoralea coryfolia, thyme oil, myrrh, and neroli extracts). The other two treatment groups received Vitilinex with UVB and NB-UVB monotherapy. After 12 weeks of topical treatment, greater than 50% repigmentation was observed in 65% receiving the topical formulation, 62% receiving NB-UVB monotherapy, and 87% receiving combination treatment, suggesting synergistic effects of the topical formulation and phototherapy. Interestingly, Psoralea coryfolia typically contained psoralens which may be synergistic with phototherapy.

In 2019, Sarac et al conducted an open-label study to analyze the efficacy of Nigella sativa seed oil on repigmentation of the face, hands, and genital regions.³⁶ They found significant pre- and post-treatment differences in 10/23 patients with facial involvement (p = 0.001), 7/16 patients with hand involvement (p = 0.005), and 7/8 patients with genital involvement (p = 0.004).³⁶ Overall, clinical studies show early evidence for the relative efficacy of herbal extract formulations in the treatment of vitiligo.

Due to its ability to prevent the accumulation of reactive oxygen species, vitamin D has similarly been studied for vitiligo management. Tang et al found that vitamin D protects human melanocytes against oxidative damage via the Wnt/β-catenin signaling activation.³⁷ A meta-analysis including 31 studies assessing serum vitamin D levels found a significantly decreased vitamin D level among vitiligo patients compared to healthy controls (standard mean difference: -1.03; p < 0.0001).³⁸ Furthermore, topical vitamin D3 has been shown to increase serum vitamin D levels.³⁹ Therefore, researchers examined the efficacy of calcipotriol, a vitamin D3 analogue, in the treatment of vitiligo.

A systematic review on the efficacy of topical calcipotriol in combination with phototherapy (either UVA, NB-UVB, or excimer laser based phototherapy) for the treatment of vitiligo uncovered that phototherapy and topical calcipotriol have synergistic effects.⁴⁰ In 2001, Ameen et al found 5/22 subjects undergoing calcipotriol 50 µg/g twice daily monotherapy to exhibit greater than 90% vitiliginous surface area reduction, although 5 subjects exhibited less than a 30% response.⁴¹ Furthermore, Chivarérini et al found no significant difference between daily topical application of calcipotriol compared to an untreated control lesion, although calcipotriol was only applied once daily.⁴² The efficacy of calcipotriol may be dose-dependent, as a study with twice-daily application found 10/14 subjects to depict improvement, although a control group was omitted.⁴³

Studies have depicted the synergistic effect of calcipotriene on other treatment regimens. For example, three studies found calcipotriol or calcipotriene treatment with betamethasone treatment to be more efficacious than calcipotriol or calcipotriene treatment alone.^44–46 Similarly, one study found combination treatment with PUVA to be more effective than calcipotriol monotherapy.⁴⁷ Additional studies assessing the efficacy of calcipotriol and tacalcitol, another vitamin D analogue, are reported in Table 1.^48–51 Interestingly, however, one case report details hyperpigmentation of freckles upon topical tacalcitol application.⁵² The results suggest that vitamin D topical monotherapy is unreliable in the treatment of vitiligo, and better results may be expected with combination therapy.

Psoralen is a naturally occurring bioactive organic compound found in the dried fruit seed of many plants,⁵³ including Angelica archangelica, Heracleum lanatum, Pastinaca saliva, and Psoralea bituminosa.⁵⁴ Psoralen is widely utilized in conjunction with phototherapy due to its ability to increase the skin’s sensitivity to light. In addition to its many sources, it is contained within Fructus Psoraleae, a plant in the family Hydrangeaceae, which has been utilized in Ayurvedic and Traditional Chinese Medicine for the treatment of osteoporosis, psoriasis, and vitiligo.⁵⁵ Anecdotal evidence for the pigment-stimulating properties of psoralen date back to the historical period, 2000 BC to 1930 AD,⁵⁶ and the combination of oral or topical psoralen with UVA therapy is commonly referred to as PUVA. However, its utility is limited by its associated side effects which may include pruritus, phototoxic reactions, erythema, itching, scaling, giddiness, nausea, and depigmented macules.⁵⁷

Oral PUVA treatment has been more frequently studied than topical PUVA. In 1997, Westerhof and Nieuweboer-Krobotova conducted an open-label study with 281 subjects to determine if topical PUVA is as efficacious as UVB radiation in the treatment of vitiligo.⁵⁸ However, they found no significant difference between treatment groups, and topical PUVA was associated with more side effects. Although prior work has demonstrated moderate efficacy with oral PUVA,⁵⁹ this study found UVB radiation to be a superior treatment option.

In 2016, a study assessed the clinical outcomes of an ointment containing Psoralea corylifolia (PC) seed powder, a source of psoralen, on repigmentation in twenty patients with vitiligo.⁶⁰ PC possesses antioxidant, antifungal, anti-inflammatory, antibacterial, anti-tumor, and immunomodulatory properties, and has therefore been used in several traditional medicines. Furthermore, it is thought to dilate capillary plexuses, increase plasma delivery at specific sites, and stimulate pigment-producing melanoblasts, which may allow for repigmentation of vitiligo-associated white lesions. Pre- and post-treatment differences in levels of pigmentation were statistically significant for small, circular white lesions of vitiligo. However, upon patch testing, mild irritation (scale-1 level) was reported in 15 subjects, and moderate irritation (scale-2 level) was reported in 5 subjects, for which betamethasone was topically applied as a counter-irritant.

A 2021 pilot study further assessed the efficacy of Psoralea corylifolia, both as a monotherapy and in combination with indicated homeopathic (IH) treatment.⁶¹ Three treatment groups existed: IH treatment only, PC treatment only, and combination treatment (IHPC). However, the IH treatment was not standardized and was instead selected on each occasion based on presenting symptoms, clinical history details, and constitutional features. Three qualified homeopaths conducted final selection of medicine for each patient, and examples of IH treatments were not provided. PC dosing regimens were based on the individual requirements of each case. All three groups exhibited a significant decrease in the Vitiligo Area Scoring Index (VASI) from baseline to month 3 and month 6, with no significant differences between groups. The PC and IHPC groups exhibited a significantly greater Vitiligo Quality of Life (VitiQoL) score than the IH group at months 3 and 6, with no significant difference between PC and IHPC. The authors concluded that all treatment regimens are equally effective and safe. Further research with larger sample sizes and the use of a true placebo or vehicle group are required to assess the efficacy of Psoralea corylifolia, although these pilot studies depict promising results for repigmentation, especially for small lesions.

Khellin has been studied as an adjunct to phototherapy in the treatment of vitiligo. Khellin is a naturally occurring furanochromone derived from the plant Amni visnaga that can be administered both orally and topically to stimulate melanocytes.³⁰ In 1998, Orecchia et al evaluated the efficacy of a khellin gel formulation in combination with topical phototherapy for the treatment of vitiligo.⁶² Thirty-six subjects with vitiligo were enrolled in the study, receiving a gel formulation consisting of water, 2-propanol, propylene glycol (WPG), and khellin on one side of the body and water, 2-propanol, propylene glycol in the absence of khellin on the other side. They found repigmentation of greater than 10% occurred in 86.1% of the khellin-WPG-treated sides, in contrast to 66.6% of the placebo-treated sides (p < 0.01). Young patients with shorter disease duration showed a better response.

In 2009, a controlled study assessed the efficacy of topical khellin 4% in combination with a monochromatic excimer light 308 nm.⁶³ Three treatment groups were included: Group I (n = 16) subjects were treated with weekly monochromatic light therapy and oral vitamin E; Group II (n = 16) subjects were treated with weekly monochromatic light therapy combined with khellin 4% ointment and oral vitamin E; and Group III (n = 16) subjects were treated solely with oral vitamin E (control). Excellent repigmentation was observed in 25% of the Group I subjects and 56.25% of the Group II subjects, and none of the Group III subjects.

In 2018, an open-label study assessed the efficacy of topical khellin in combination with a 308 nm excimer lamp among twenty patients with resistant vitiligo.⁶⁴ They observed excellent repigmentation (greater than 75%) in 9/20 subjects, good repigmentation (50-75%) in 5/20 subjects, moderate repigmentation (25-50%) in 3/20 subjects, and poor repigmentation (less than 25%) in 3/20 subjects. Furthermore, no recurrences were observed six months after treatment. Although this open-label study omitted a control group, the authors concluded that the combination of 308 nm excimer lamp treatment with topical khellin is a safe and effective treatment for vitiligo; however, larger trials are required to confirm these results.

A 2004 study sought to directly compare local khellin and UVA (KUVA) with systemic PUVA treatment.⁶⁵ The pilot study included 33 patients, and the results indicated that local KUVA treatment required longer duration and higher UVA doses, and better KUVA results were achieved with younger patients. Yet, no patient treated with KUVA experienced any adverse effects. In contrast, some patients treated with PUVA developed erythema, itching, and gastro-intestinal disturbances. These results demonstrate that local KUVA treatment may be better tolerated than systemic PUVA treatment, although patients may require greater treatment duration to achieve the same degree of repigmentation as with PUVA. Additional studies have similarly depicted the efficacy of KUVA phototherapy,⁶⁶ highlighting its equitable efficacy compared to psoralens. Future research with a greater sample size is required to confirm such findings. Yet, these small studies show promising results.

In 2007, a randomized study including 100 subjects with vitiligo was conducted to assess the efficacy of an antioxidant and mitochondrial stimulating topical formula for use in hypopigmented areas for five months.⁶⁷ Five treatment groups were included in the analysis: Group 1 received oral antioxidants and phenylalanine in addition to the topical formulation; Group 2 received oral antioxidants and phenylalanine in addition to a placebo cream; Group 3 received oral antioxidants and phenylalanine only; Group 4 received a placebo cream only; and Group 5 received the topical antioxidant formulation only. Oral antioxidants included vitamin C, vitamin E, zinc, selenium, magnesium, and coenzyme Q10. Average clinical pigmentation was scored according to an 11-point scale, with 0 points indicating the absence of pigment and 11 points indicating pigment in more than 11 mm. Group 1 (oral antioxidants and phenylalanine in addition to the topical formulation) subjects exhibited the greatest repigmentation (average score of 10.4, p < 0.001), followed by Group 5 (receiving just the topical formulation) subjects, (average score of 9.77, p < 0.001). Groups 2 and 3 scores were 1.23 and 1.16, respectively, which were significantly higher than group 4, the placebo group (score of 0.08). The clinical and histological responses of both Groups 1 and 5 were significantly greater than any other group. Thus, the topical antioxidant formulation demonstrated efficacious results, further potentiated by oral administration of antioxidants and phenylalanine.

In 2016, Soliman et al assessed the efficacy of a topical antioxidant hydrogel with excimer light therapy in comparison to excimer light monotherapy.⁶⁸ The hydrogel consisted of SOD, copper, zinc, vitamin B12, and calcium pantothenate. Thirty subjects were included in the study, and 2-4 stable vitiliginous lesions of each subject were selected and divided into two groups. On each patient, group A lesions received the combination therapy, group B lesions received excimer light monotherapy only, and one lesion was left untreated as a control. Lesions were treated twice a week, up to 24 sessions. Group A lesions, receiving the topical antioxidant hydrogel along with excimer monotherapy showed greater repigmentation than Group B (p < 0.001). Of the lesions in Group A, 20% achieved excellent repigmentation, 26.7% achieved good repigmentation, 22.2% achieved moderate repigmentation, and 22.2% achieved poor repigmentation. In contrast, no Group B lesions achieved excellent or good repigmentation, with 48.9% exhibiting moderate repigmentation and 42.4% exhibiting poor repigmentation.

An additional pilot study evaluated the effect of an antioxidant cream versus placebo in combination with a 308 nm excimer laser. The antioxidant cream contained folic acid, phenylalanine, sitosterol, hyaluronic acid, Mexican bamboo extract, Chilean boldo tree boldine, aminoguanidine HCl, and decarboxy carnosine HCl. Ten vitiligo patients with symmetrical vitiliginous lesions were included in the study. Lesions treated with topical antioxidant hydrogel demonstrated greater and faster repigmentation than lesions treated with the vehicle control, further supporting the adjunct effect of topical antioxidants with systemic treatments or phototherpy.⁶⁹ Repigmentation was recorded according to a five-point scale (0 = no repigmentation, 1 = up to 25% repigmentation, 2 = 26-50% repigmentation, 3 = 51-75% repigmentation, and 4 = 76-100% repigmentation). At month 3, lesions treated with the antioxidant hydrogel exhibited a repigmentation grade of 3.30 ± 0.67, compared to a repigmentation grade of 2.60 ± 0.7 in lesions treated with the placebo cream (p < 0.01). Four additional topical formulations with antioxidant properties are listed in Table 1.^70–73

In 2015, Djerrou published a case report detailing the successful treatment of vitiligo using a formulation including honeybee Allium cepa and Avena sativa, coupled with sunlight exposure.⁷⁴ The patient achieved complete repigmentation of white vitiliginous lesions with no adverse effects. However, because phototherapy is efficacious for vitiligo, it is not clear if the formulation would have worked in the absence of sun exposure since they were used together.

Janus kinase (JAK) inhibitors are a novel class of anti-inflammatory molecules that represent the first topical medication that has been specifically FDA-approved for use in vitiligo. There is interest within the integrative dermatology space to use topical JAK inhibitors as a non-steroidal alternative.

The JAK signal transducer and activator of transcription (STAT) pathway foster cytokine-mediated signal transduction of inflammatory mediators. Together with IFN-γ (a type-II interferon), the JAK/STAT signaling pathway is implicated in the pathogenesis of vitiligo⁷⁵; mouse vitiligo studies have suggested that the positive IFN-γ-chemokine axis feedback loop may allow the initiation and progression of vitiligo.⁷⁵ IFN-γ activates the JAK/STAT1 pathway, resulting in STAT1 phosphorylation and gene transcription. However, IFN-γ can be blocked by the inhibition of JAK1 or JAK2, suggesting that this pathway may have great pharmacologic potential in the management of vitiligo.

Oral tofacitinib is a JAK inhibitor that has been used off-label for the treatment of vitiligo with reported success.^76,77 Recent studies have similarly assessed the efficacy of topical formulations. In 2019, Owens et al conducted a study to assess the effect of ruxolitinib cream on inflammatory profiles in patients with vitiligo, providing molecular support for its use in the treatment of vitiligo.⁷⁸ Of 1,104 proteins assessed, 204 proteins exhibited significantly modulated expression (p < 0.05) in the 1.5% twice-daily treatment group; 162 proteins in the 1.5% once-daily group, 71 proteins in the 0.5% once-daily group, 29 proteins in the 0.15% once-daily group, and 56 proteins in the vehicle control group exhibited significant expression modulation. Furthermore, chemokine C-X-C Motif Chemokine Ligand 10 (CXCL10), implicated in vitiligo pathogenesis by T cell recruitment to the site of inflammation, was significantly downregulated in both 1.5% twice-daily and once-daily treatment groups. This study provided evidence for the dose-dependent nature of ruxolitinib-associated inflammatory mediation.

Research has further depicted clinical efficacy. Rothstein et al evaluated twice-daily topical ruxolitinib 1.5% among 12 patients in an open-label proof-of-concept trial.⁷⁹ Nine subjects completed the study for the 20-week duration. Overall, Vitiligo Area Scoring Index scores improved 23% in enrolled patients at week 20 (95% confidence interval: 4-43%; p = 0.02). Furthermore, four patients who had significant facial vitiliginous involvement experienced 76% improvement in facial Vitiligo Area Scoring Index scores at week 20 (95% confidence interval: 53-99%; p = 0.001).

The site-specificity of response is demonstrated by a subgroup analysis from a phase 2, randomized, double-blind trial.⁸⁰ 157 subjects were included in the initial study, although the subgroup analysis included 33 patients with vitiligo affecting less than or equal to 20% of total body surface area (T-BSA), as ruxolitinib application was limited to ≤ 20% T-BSA for practicality and safety.⁸¹ 60% of head and neck lesions experienced greater than 50% improvement in total Vitiligo Area Scoring Index (T-VASI50). 52.9% of upper extremity lesions, 52.6% of lower extremity lesions, 29.4% of foot lesions, and 15.0% of hand lesions experienced greater than 50% response. Whereas the initial trial showed the relative efficacy of topical ruxolitinib cream in the treatment of facial and total body vitiligo,⁸¹ the sub-group analysis found site-specific differential responses.

In addition to topical ruxolitinib, topical tofacitinib has also been studied among vitiligo patients. In 2020, Mobasher et al conducted an open-label pilot study to evaluate the clinical efficacy of topical 2% tofacitinib cream among 16 patients with vitiligo, 11 of which had generalized vitiligo.⁸² Four patients experienced greater or equal to 90% repigmentation, five patients experienced 25-75% repigmentation, four patients experienced 5-15% repigmentation, and three patients did not experience repigmentation. Like ruxolitinib, the topical tofacitinib cream was significantly more effective on facial lesions than non-facial lesions (p = 0.022). Furthermore, greater improvement was observed on patients with Fitzpatrick skin types IV-VI (p = 0.034).

McKesey and Pandya similarly reported a pilot study involving 11 patients who received 2% tofacitinib cream twice daily in combination with NB-UVB for treatment of facial vitiligo.⁸³ The authors noted good to excellent repigmentation in all 11 patients. It is likely that this study observed more efficacious results than that reported by Mobasher et al as studied lesions were confined to the face.⁸² McKensey and Pandya concluded that topical tofacitinib and phototherapy synergistically can lead to improvement of vitiligo. This observation aligns with two case reports published by Joshipura et al supporting the importance of light in the treatment of vitiligo with JAK inhibitors.⁸⁴ Interestingly, however, Mobasher et al state that their case series failed to depict a clear pattern regarding concomitant phototherapy.⁸² Larger, controlled trials are necessary to determine the efficacy of topical tofacitinib monotherapy compared to combination with phototherapy.

Although topical ruxolitinib and tofacitinib are the most frequently studied topical JAK inhibitors for the treatment of vitiligo, Yagi et al reported two cases of vitiligo treated with delgocitinib, albeit with mixed results.⁸⁵ Although no adverse effects were observed in either case, only one case demonstrated significant repigmentation upon topical application. However, the successful case involved treatment of the neck, whereas the unsuccessful case involved treatment of the elbow. As previously described, site-specific differences in response have been observed with topical JAK inhibitors, which may have contributed to the differing results presented by Yagi et al. Additional studies assessing the efficacy of topical JAK inhibitors are listed in Table 1.^86–89

An open-label study compared the efficacy of Bimatoprost 0.01% twice daily application to Tacrolimus 0.1% twice daily for twenty weeks (n = 10 subjects with two or more vitiliginous lesions).⁹⁰ They found the total vitiliginous lesion surface area to decrease from baseline (p < 0.05), although with no significant difference compared to Tacrolimus 0.1%. The bimatoprost 0.01% and the tacrolimus 0.1% groups achieved greater than 50% repigmentation at 12 weeks in 20% and 10% of subjects, respectively. Itching and burning were similarly reported with both bimatoprost 0.01% and Tacrolimus 0.1%.

In contrast, a 2016 study utilized a greater concentration of bimatoprost. Bimatoprost 0.03% was assessed for its efficacy in vitiligo response, both as a monotherapy and in combination with mometasone.⁹¹ Mometasone plus placebo was utilized as a control group. Thirty-two patients were randomized into one of the groups and a response was defined as 25%-50% global improvement. 46% of patients receiving bimatoprost plus mometasone were found to have a response, compared to 18% of patients receiving bimatoprost monotherapy and 0% receiving mometasone plus placebo. The results indicate a synergistic effect of bimatoprost 0.03% and mometasone administration, although few lesions exhibited repigmentation greater than 50%. There were no differences in signs and symptoms of irritation among groups.

Lastly, a 2021 study evaluated the efficacy of either bimatoprost 0.01% solution or placebo solution plus once-monthly fractional carbon dioxide laser with twice-weekly NB-UVB therapy.⁹² Fifteen subjects were included in the analysis, each with paired vitiliginous lesions that could be randomized to each treatment group. At week 12, the percent change in melanin concentration from baseline was greater on lesions receiving bimatoprost 0.1% (27.17 ± 13.62% vs. 22.82 ± 10.10% p = 0.028). A greater change in vitiligo surface area was observed among lesions receiving bimatoprost 0.01% than placebo, but the changes were not statistically significant.

These studies demonstrate the moderate efficacy of bimatoprost in the treatment of vitiligo, while highlighting potential synergistic effects of combination therapies. Additional studies with greater sample sizes are required to determine if bimatoprost 0.01% can effectively be used as a monotherapy, or if laser and/or NB-UVB supplemental therapy is required. Furthermore, additional studies are required to determine if efficacious results may similarly be observed for vitiliginous lesions of the face.

RKS serves as a scientific advisor for LearnHealth, Codex Labs Corp, and Arbonne and as a consultant to Burt’s Bees, Novozymes, Nutrafol, Incyte, Fotona, Element Apothec, Abbvie, Leo, UCB, Sun, Sanofi, Regeneron Pharmaceuticals. JM serves as a consultant for Codex Labs Corp. The other authors report no conflicts.

N/A.

EH: Ecliptae herba

JAK: Janus kinase

JAK/STAT: Janus kinase/ signal transducer and activator of transcription

KUVA: Khellin-UVA

NB-UVB: Narrowband UVB

PMRP: Polygoni multiflora radix praeparata

PUVA: Psoralens-UVA

RRP: Rehmanniae radix praeparata

T-VASI50: >50% Improvement in total Vitiligo Area Scoring Index

T-VASI75: >75% Improvement in total Vitiligo Area Scoring Index

SOD: Superoxide dismutase