Vitiligo.Care & specialists in India

No. Vitiligo is an autoimmune disease in which the body's own immune system destroys melanocytes. It cannot be passed by skin contact, sharing clothes, sharing food, swimming pools, or any other means. Family clustering reflects shared genetic risk for autoimmunity, not transmission.

Vitiligo is caused by CD8+ T cells attacking and destroying epidermal melanocytes through interferon-gamma signalling. Genetic susceptibility (over 50 risk loci, including HLA, NLRP1, and PTPN22), oxidative stress within melanocytes, skin trauma (the Koebner phenomenon), and major psychological stress all contribute to triggering and progression in susceptible individuals.

Vitiligo is not curable in the sense that the underlying autoimmune tendency persists, but it is increasingly treatable. Topical ruxolitinib, narrowband UVB, topical corticosteroids and calcineurin inhibitors, and surgical techniques restore meaningful pigment in the majority of motivated patients with non-segmental disease. Maintenance therapy reduces relapse rates from around 40-50% to under 10% at one year.

Vitiligo is a clinical diagnosis made by a dermatologist on examination. The hallmark is sharply demarcated milk-white patches that fluoresce bright bluish-white under a Wood's lamp in a dark room. Atypical cases are confirmed by skin biopsy showing absence of melanocytes. Blood tests for thyroid antibodies and vitamin B12 are routinely added because of autoimmune comorbidity.

Non-segmental vitiligo is bilateral, symmetric, and chronic with active and stable phases; it accounts for 70-80% of cases and is strongly autoimmune-mediated. Segmental vitiligo is unilateral, follows a band-like distribution, usually starts in childhood, progresses rapidly for 1-2 years and then stabilizes. Segmental disease responds best to surgical treatment.

In the phase 3 TRuE-V1 and TRuE-V2 trials, topical ruxolitinib 1.5% cream achieved at least 50% facial repigmentation in roughly 30% of patients at 24 weeks and in 50% by 52 weeks. Total-body 50% repigmentation was reached by about 20% at 24 weeks. The cream is approved for non-segmental vitiligo from age 12 with up to 10% body surface coverage.

Narrowband UVB delivers a narrow band of ultraviolet B light at 311-313 nm in a dermatology clinic phototherapy unit, two to three times a week for 6-12 months. It suppresses cutaneous T cells and stimulates melanocyte migration from hair follicles into depigmented skin. It achieves at least 25% repigmentation in 60-75% of patients with non-segmental disease.

No diet cures vitiligo. There is no evidence that any specific food causes or eliminates the disease. A balanced anti-inflammatory dietary pattern rich in coloured vegetables, fruits, and oily fish supports general health and antioxidant defences, but it does not replace topical therapy, phototherapy, or surgical treatment.

Yes. Autoimmune thyroid disease, especially Hashimoto thyroiditis, affects 15-20% of adults with vitiligo compared with around 5% in the general adult population. Annual TSH plus anti-TPO antibody screening is standard care, with more frequent testing in children and any patient with new fatigue, weight change, or temperature intolerance.

Yes, to a degree. About 20-25% of patients have an affected first-degree relative. Twin studies show roughly 23% concordance in identical twins, indicating a strong but incomplete genetic component. Risk is polygenic rather than simple Mendelian, and lifetime environmental triggers (stress, trauma, chemicals) determine if and when the disease declares itself.

Yes. Roughly half of all vitiligo cases begin before age 20 and about 25% before age 10. Childhood vitiligo includes a higher proportion of segmental disease and carries a substantial psychosocial burden. Topical tacrolimus or pimecrolimus, narrowband UVB, and 308 nm excimer laser are well-established treatments in paediatric dermatology.

Both. Controlled medical UVB exposure in a phototherapy unit stimulates repigmentation and is a cornerstone of treatment. Uncontrolled outdoor sun causes sunburn and Koebner spread on melanocyte-free patches and increases long-term skin cancer risk. Daily broad-spectrum sunscreen SPF 30-50 on uncovered skin is essential for every vitiligo patient.

Major psychological stress precedes onset or worsening of vitiligo in roughly 60% of patient series. Stress is not the only cause, but in genetically susceptible people it can shift cutaneous immunity toward autoimmune attack. Structured stress management, cognitive behavioural therapy, or mindfulness-based approaches measurably improve overall outcomes.

Loss of pigment in eyelashes, eyebrows, or scalp hair within a vitiligo patch is called leukotrichia. It reflects destruction of follicular melanocytes, which act as the reservoir for repigmentation. Leukotrichia at a site predicts a poorer repigmentation response there because the reservoir is depleted; surgical techniques may be needed for cosmetic restoration.

Generalized non-segmental vitiligo can progress over years and in a minority of patients reaches the universal stage with more than 80% body involvement. Rapid spread is more common during active phases with confetti-like depigmentation and Koebner phenomenon. Early treatment during active phases substantially reduces the chance of extensive progression.

First signs of repigmentation typically appear after 8-12 weeks of consistent therapy as small dotted islands of pigment around hair follicles within a patch. Visible shrinkage of patches develops over 3-6 months with topical therapy and 4-8 months with phototherapy. Maximum response is usually reached at 12-18 months of continuous treatment.

Relapse occurs in roughly 40-50% of patients within 12 months of stopping active therapy. Proactive maintenance therapy with topical tacrolimus 0.1% ointment applied twice weekly to previously affected sites reduces 12-month relapse rates to under 10% in randomized data (Cavalié 2015). Sun protection, stress management, and ongoing dermatology follow-up are essential.

There is no vaccine. Approved pharmacotherapy for non-segmental vitiligo currently includes topical ruxolitinib 1.5% cream (FDA-approved 2022). Oral JAK inhibitors and other systemic therapies are in active phase 3 trials and may become available in the next several years. Oral mini-pulse corticosteroids are used off-label for rapidly progressing disease.

Vitiligo itself does not shorten life expectancy. It can affect quality of life substantially, and associated autoimmune diseases such as thyroid disorders and type 1 diabetes have their own implications. Regular screening for autoimmune comorbidity, sun protection on melanocyte-free skin, and mental health support are part of standard long-term care.

Tattooing carries a real risk of triggering new vitiligo patches at the tattoo site through the Koebner phenomenon, particularly in active disease. Medical micropigmentation by a trained practitioner can camouflage stable patches but is not first-line and should be discussed with a dermatologist after disease has been stable for at least 12 months.

No. Vitiligo is an autoimmune disease, not a cancer. Paradoxically, large cohort studies suggest a slightly lower overall risk of melanoma and non-melanoma skin cancer in vitiligo patients, possibly reflecting overlapping immune surveillance. Sun protection of depigmented skin remains essential because individual patches lack melanin defence against UV damage.

See a dermatologist for any new depigmented patch that does not resolve within a few weeks, especially on the face, hands, or genitals, or if patches are spreading rapidly, if eyelashes or eyebrows are turning white inside patches, or if first-line topical therapy fails after 3 months. Specialist input is essential before starting phototherapy, oral steroids, or surgery.