Vitiligo
Vitiligo | |
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Specialty | Dermatology |
Vitiligo /ˌvɪt[invalid input: 'ɨ']ˈlaɪɡoʊ/ is a condition that causes depigmentation of parts of the skin. It occurs when melanocytes, the cells responsible for skin pigmentation, die or are unable to function. The cause of vitiligo is unknown, but research suggests that it may arise from autoimmune, genetic, oxidative stress, neural, or viral causes.[1] The incidence worldwide is less than 1%.[2] There are two main types of vitiligo: idiopathic and chemical.[3] Most vitiligo is idiopathic, however in cases where it is triggered by skin bleaching or other substances, it is said to be chemical.
Signs and symptoms
The most notable symptom of vitiligo is depigmentation of patches of skin that occurs on the extremities.[4][5] Although patches are initially small, they often enlarge and change shape.[1][4] When skin lesions occur, they are most prominent on the face, hands and wrists.[4][5] Depigmentation is particularly noticeable around body orifices, such as the mouth, eyes, nostrils, genitalia and umbilicus.[4][5] Some lesions have hyperpigmentation around the edges.[6] Patients who are stigmatised for their condition may experience depression and similar mood disorders.[7] A Black light (also referred to as a UVA light, Wood's lamp, or simply ultraviolet light) can be used in the early phase of this disease for identification and to determine effectiveness of treatment. Skin with vitiligo, when exposed to a black light, will glow yellow, green or blue, in contrast to healthy skin which will have no reaction.
Cause
Non-segmental
In non-segmental vitiligo (NSV), there is usually some form of symmetry in the location of the patches of depigmentation. New patches also appear over time and can be generalized over large portions of the body or localized to a particular area. Vitiligo where little pigmented skin remains is referred to as vitiligo universalis. NSV can come about at any age (unlike segmental vitiligo, which is far more prevalent in teenage years).[6]
Classes of non-segmental vitiligo include:
- Generalized Vitiligo: the most common pattern, wide and randomly distributed areas of depigmentation[8]
- Universal Vitiligo: depigmentation encompasses most of the body[8]
- Focal Vitiligo: one or a few scattered macules in one area, most common in children[8]
- Acrofacial Vitiligo: fingers and periorificial areas[8]
- Mucosal Vitiligo: depigmentation of only the mucous membranes[8]
Segmental
Segmental vitiligo (SV) differs in appearance, etiology and prevalence from associated illnesses. Its treatment is different from that of NSV. It tends to affect areas of skin that are associated with dorsal roots from the spine and is most often unilateral. It spreads much more rapidly than NSV and, without treatment, it is much more stable/ static in course and is not associated with auto-immune diseases. It is a very treatable condition that responds to topical treatment.[6]
Differential diagnosis
Conditions with similar symptoms include:
- Pityriasis alba
- Tuberculoid leprosy
- Postinflammatory hypopigmentation
- Tinea versicolor[8]
- Albinism
- Piebaldism[8]
- Idiopathic guttate hypomelanosis[8]
- Progressive macular hypomelanosis[8]
- Primary adrenal insufficiency
Pathogenesis
Vitiligo is a disorder characterized by patchy loss of skin pigmentation due to immune attacks on melanocytes. Although there is no significant proof or evidence, many doctors believe that it can be caused by defects in many genes.[citation needed] Variations in genes that are part of the immune system or part of melanocytes have both been associated with vitiligo. The immune system genes are associated with other autoimmune disorders.
In one case, the gene TYR, which makes the melanocyte more susceptible to the immune system in vitiligo, also makes the melanocyte more susceptible to the immune system in the skin cancer malignant melanoma. Therefore, people with vitiligo caused by the TYR gene are less likely to have malignant melanoma.
A genomewide association study found 10 independent susceptibility loci for generalized vitiligo, responsible for 7.4% of the genetic risk. Some patients had vitiligo alone; others had generalized vitiligo with other autoimmune diseases. Most loci were associated with both forms. (The exception was PTPN22, which was only associated with generalized vitiligo.) In the major histocompatibility complex (MHC) region, which controls the immune system, major association signals were identified in the class I gene region (between HLA-A and HLA-HGC9) and class II gene region (between HLA-DRB1 and HLA-DQA1). Outside the MHC region, association signals were identified near RERE, PTPN22, LPP, IL2RA, GZMB, UBASH3A and C1QTNF6 genes, which are associated with other autoimmune diseases. TYR encodes tyrosinase, which is not a component of the immune system, but is an enzyme of the melanocyte that catalyzes melanin biosynthesis, and a major autoantigen in generalized vitiligo. The major alleles of TYR are associated with vitiligo, and the minor alleles are associated with malignant melanoma. Vitiligo-associated 402R tyrosinase may be more efficiently presented to the immune system. Melanoma-associated 402Q may fail to be identified by the immune system.[9]
The transcriptional profile of melanocytes from vitiligo patients have been studied. Oligonucleotide microarrays containing approximately 16,000 unique genes were used to analyse mRNA expression in melanocytes from vitiligo patients and age-matched healthy controls. In total, 859 genes were identified as differentially expressed.[10]
Vitiligo is sometimes associated with autoimmune and inflammatory diseases,[11] commonly thyroid overexpression and underexpression. A study comparing 656 people with and without vitiligo in 114 families found several mutations (single-nucleotide polymorphisms) in the NALP1 gene. The NALP1 gene, which is on chromosome 17 located at 17p13, is on a cascade that regulates inflammation and cell death, including myeloid and lymphoid cells, which are white cells that are part of the immune response. NALP1 is expressed at high levels in T cells and Langerhan cells, white blood cells that are involved in skin autoimmunity. Polymorphisms of CD4 were shown to be associated with the vitiligo and other autoimmune diseases like type I Diabetes Mellitus.[12]
Among the inflammatory products of NALP1 are caspase 1 and caspase 7, which activate the inflammatory cytokine interleukin-1β. Interleukin-1β is expressed at high levels in patients with vitiligo. Some compounds inhibit caspase and interleukin-1β, and so might be useful drugs for vitiligo and associated autoimmune diseases. In one of the mutations, the amino acid leucine in the NALP1 protein was replaced by histidine (Leu155->His). The original protein and sequence is highly conserved in evolution, and found in humans, chimpanzee, rhesus monkey, and bush baby, which means that it is an important protein and an alteration is likely to be harmful. Addison's disease (typically an autoimmune destruction of the adrenal glands) may cause vitiligo.[13][14]
Treatment
There are a number of treatments for vitiligo with the best evidence for applied steroids and the combination of ultraviolet light in combination with creams.[15] Due to the higher risks of skin cancer, the NHS suggests phototherapy only be used if primary treatments are ineffective.[16]
Phototherapy
Exposing the skin to UVB light from UVB lamps is the most common treatment for vitiligo. The treatments can be done at home with a domestic UVB lamp or in a clinic. It is important to control the exposure time so that the skin does not burn from overexposure. Treatment can take a few weeks if the spots are on the neck and face and if they existed not more than 3 years. If the spots are on the hands and legs and have been there more than 3 years, it can take a few months. In a clinic the treatments are done 2–3 times a week, and at home every day, which makes the home treatments more effective. Spots on a large area of the body may require full body treatment in a clinic or hospital. Both UVB broadband and UVB narrowband lamps can be used.[17][18] However, these treatments are unreliable at best.[citation needed] There is no treatment that totally repigments the skin. Adding a psoralen, a photosensitizer, or an immunomodulant[19] that increases the effect of the UV light can aid in partial repigmentation.
A 1997 report suggests that combining vitamin B12 and folic acid supplements with sun exposure caused repigmentation in 52% of cases.[20]
Ultraviolet light (UVA) treatments are normally carried out in a hospital clinic.Psoralen and ultraviolet A light (PUVA) treatment involves taking a drug that increases the skin's sensitivity to ultraviolet light, then exposing the skin to high doses of UVA light. Treatment is required twice a week for 6–12 months or longer. Because of the high doses of UVA and psoralen, PUVA may cause side effects such as sunburn-type reactions or skin freckling.[16]
Narrowband ultraviolet B (UVB) phototherapy is now used more commonly than PUVA as it is less damaging to the skin. As with PUVA, treatment is carried out twice weekly in a clinic or every day at home, and there is no need to use psoralen.[16]
Immune mediators
Tentative evidence supports a role for tacrolimus.[21] There is tentative short term evidence for pimecrolimus but long term data is missing.[22]
Skin camouflage
In mild cases, vitiligo patches can be hidden with makeup or other cosmetic camouflage solutions. If the affected person is pale-skinned, the patches can be made less visible by avoiding tanning of affected skin.[8]
De-pigmenting
In cases of extensive vitiligo the option to de-pigment the unaffected skin with topical drugs like monobenzone, mequinol, or hydroquinone may be considered to render the skin an even colour. The removal of all the skin pigment with monobenzone is permanent and vigorous. Sun-safety must be adhered to for life to avoid severe sun burn and melanomas. Depigmentation takes about a year to complete.[16]
Transplanting melanocytes
In October 1992, a scientific report was published of successfully transplanting melanocytes to vitiligo affected areas, effectively repigmenting the region.[23] The procedure involved taking a thin layer of pigmented skin from the patient's gluteal region. Melanocytes were then separated out to a cellular suspension that was expanded in culture. The area to be treated was then denuded with a dermabrader and the melanocytes graft applied. Between 70 and 85 percent of patients experienced nearly complete repigmentation of their skin. The longevity of the repigmentation differed from person to person.[24]
Notable cases
- Michael Jackson announced publicly in a 90-minute interview with Oprah Winfrey in February 1993 that he had vitiligo.[25] This was confirmed by the autopsy report following his death in 2009.[26]
- Jon Hamm reported developing stress-induced vitiligo while working on the series Mad Men.[27]
- UFC fighter Scott Jorgensen suffers from a particularly aggressive form of the disease and has received the unnofficial nickname 'Spotty' as a result of the appearance it causes his skin to have. In 2012 Jorgensen claimed to have allowed the disease to "pretty much take over" and as a result give his skin a uniform colour.[28]
- Model and America’s Next Top Model contestant Chantelle Brown-Young has an aggressive form of vitiligo. The condition hasn't deterred her from her modeling career and Chantelle has become a “vitiligo spokesmodel”.[29]
See also
References
- ^ a b Halder, RM; Chappell, JL (2009). "Vitiligo update". Seminars in cutaneous medicine and surgery. 28 (2): 86–92. doi:10.1016/j.sder.2009.04.008. PMID 19608058.
- ^ Nath SK, Majumder PP, Nordlund JJ (1994). "Genetic epidemiology of vitiligo: multilocus recessivity cross-validated". American Journal of Human Genetics. 55 (5): 981–90. PMC 1918341. PMID 7977362.
{{cite journal}}
: CS1 maint: multiple names: authors list (link) - ^ Fisher's Contact Dermatitis by Alexander Fisher, pg 470
- ^ a b c d National Institute of Arthritis and Musculoskeletal and Skin Diseases (March 2007). "What Is Vitiligo? Fast Facts: An Easy-to-Read Series of Publications for the Public Additional". Retrieved 18 July 2010.
- ^ a b c Halder RM; et al. (2007). "72. Vitiligo". In Wolff K, Freedberg IM, Fitzpatrick TB (eds) (ed.). Fitzpatrick's dermatology in general medicine (7th ed.). New York: McGraw-Hill Professional. ISBN 978-0-07-146690-5. OCLC 154751587.
{{cite book}}
:|editor=
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(help)CS1 maint: multiple names: editors list (link) - ^ a b c Huggins RH, Schwartz RA, Janniger CK (2005). "Vitiligo" (PDF). Acta Dermatovenerologica Alpina, Panonica, et Adriatica. 14 (4): 137–42, 144–5. PMID 16435042.
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: CS1 maint: multiple names: authors list (link) - ^ Picardi A, Pasquini P, Cattaruzza MS, Gaetano P, Melchi CF, Baliva G, Camaioni D, Tiago A, Abeni D, Biondi M (2003). "Stressful life events, social support, attachment security and alexithymia in vitiligo. A case-control study". Psychotherapy and Psychosomatics. 72 (3): 150–8. doi:10.1159/000069731. PMID 12707482.
{{cite journal}}
: CS1 maint: multiple names: authors list (link) - ^ a b c d e f g h i j Halder RM, et al. Vitiligo. In: Wolff K, et al. Fitzpatrick's Dermatology in General Medicine. 7th ed. New York, N.Y.: McGraw-Hill Professional; 2007
- ^ Jin Y, Birlea SA, Fain PR; et al. (2010). "Variant of TYR and Autoimmunity Susceptibility Loci in Generalized Vitiligo". N. Engl. J. Med. 362 (18): 1686–97. doi:10.1056/NEJMoa0908547. PMC 2891985. PMID 20410501.
{{cite journal}}
: Explicit use of et al. in:|author=
(help)CS1 maint: multiple names: authors list (link) - ^ Strömberg S, Björklund MG, Asplund A; et al. (2008). "Transcriptional profiling of melanocytes from patients with vitiligo vulgaris". Pigment Cell & Melanoma Research. 21 (2): 162–71. doi:10.1111/j.1755-148X.2007.00429.x. PMID 18426409.
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: Explicit use of et al. in:|author=
(help)CS1 maint: multiple names: authors list (link) - ^ Hedstrand H, Ekwall O, Olsson MJ; et al. (2001). "The transcription factors SOX9 and SOX10 are vitiligo autoantigens in autoimmune polyendocrine syndrome type I". The Journal of Biological Chemistry. 276 (38): 35390–5. doi:10.1074/jbc.M102391200. PMID 11423552.
{{cite journal}}
: Explicit use of et al. in:|author=
(help)CS1 maint: multiple names: authors list (link) CS1 maint: unflagged free DOI (link) - ^ Mashaghi A; et al. (2010). "Possible association of the CD4 gene polymorphism with vitiligo". Clin Exp Dermatol. 35 (5): 521–4. doi:10.1111/j.1365-2230.2009.03667.x. PMID 19843086.
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: Explicit use of et al. in:|author=
(help) - ^ Gregersen PK (2007). "Modern genetics, ancient defenses, and potential therapies". The New England Journal of Medicine. 356 (12): 1263–6. doi:10.1056/NEJMe078017. PMID 17377166.
- ^ Jin Y, Mailloux CM, Gowan K; et al. (2007). "NALP1 in vitiligo-associated multiple autoimmune disease". The New England Journal of Medicine. 356 (12): 1216–25. doi:10.1056/NEJMoa061592. PMID 17377159.
{{cite journal}}
: Explicit use of et al. in:|author=
(help)CS1 maint: multiple names: authors list (link) - ^ Whitton, ME (October 2008). "Therapeutic interventions for vitiligo". Journal of the American Academy of Dermatology. 59 (4): 713–7. doi:10.1016/j.jaad.2008.06.023. PMID 18793940.
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ignored (|author=
suggested) (help) - ^ a b c d Anon. "Vitiligo -Treatment". Patient UK. NHS. Retrieved 3 June 2013.
- ^ Scherschun, L; Kim, JJ; Lim, HW (2001). "Narrow-band ultraviolet B is a useful and well-tolerated treatment for vitiligo". Journal of the American Academy of Dermatology. 44 (6): 999–1003. doi:10.1067/mjd.2001.114752. PMID 11369913.
- ^ Don, Philip; Iuga, Aurel; Dacko, Anne; Hardick, Kathleen (2006). "Treatment of vitiligo with broadband ultraviolet B and vitamins". International Journal of Dermatology. 45 (1): 63–5. doi:10.1111/j.1365-4632.2005.02447.x. PMID 16426381.
- ^ Nisticò S, Chiricozzi A, Saraceno R, Schipani C, Chimenti S (January 2012). "Vitiligo treatment with monochromatic excimer light and tacrolimus: results of an open randomized controlled study". Photomed Laser Surg. 30 (1): 26–30. doi:10.1089/pho.2011.3029. PMID 22054204.
{{cite journal}}
: CS1 maint: multiple names: authors list (link) - ^ Juhlin L, Olsson MJ (1997). "Improvement of vitiligo after oral treatment with vitamin B12 and folic acid and the importance of sun exposure". Acta Derm. Venereol. 77 (6): 460–2. PMID 9394983.
- ^ Tjioe, M (2006). "Topical macrolide immunomodulators: a role in the treatment of vitiligo?". American journal of clinical dermatology. 7 (1): 7–12. doi:10.2165/00128071-200607010-00002. PMID 16489839.
{{cite journal}}
: Unknown parameter|coauthors=
ignored (|author=
suggested) (help) - ^ Boone, B (January–February 2007). "Topical pimecrolimus in the treatment of vitiligo". European journal of dermatology : EJD. 17 (1): 55–61. PMID 17324829.
{{cite journal}}
: Unknown parameter|coauthors=
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suggested) (help) - ^ Olsson MJ, Juhlin L (1992). "Melanocyte transplantation in vitiligo". Lancet. 340 (8825): 981. doi:10.1016/0140-6736(92)92875-G. PMID 1357390.
- ^ Olsson MJ, Juhlin L (2002). "Long-term follow-up of leucoderma patients treated with transplants of autologous cultured melanocytes, ultrathin epidermal sheets and basal cell layer suspension". The British Journal of Dermatology. 147 (5): 893–904. doi:10.1046/j.1365-2133.2002.04837.x. PMID 12410698.
- ^ Hutchison, Courtney. "Like Father, Like Son? Prince Michael Appears to Have Vitiligo". ABC News. Retrieved 16 April 2013.
- ^ Duke, Alan (7 May 2013). "Autopsy reveals Michael Jackson's secrets". CNN Entertainment. CNN. Retrieved 7 May 2013.
The autopsy confirmed what Jackson told people who questioned why his skin tone became lighter in the 1980s. Jackson had 'vitiligo, a skin pigmentation disease,' [LA coroner Dr. Christopher] Rogers said. 'So, some areas of the skin appear light and others appear dark.'
- ^ "Mad Men star Jon Hamm blames skin disease on stress | Don Draper". Theage.com.au. Retrieved 11 February 2014.
- ^ "Scott Jorgensen's extreme Vitiligo solution". mixedmartialarts.com. Retrieved 7 April 2014.
- ^ Taylor, Victoria (8 May 2014). New York Daily News http://www.nydailynews.com/life-style/health/top-model-contestant-hasn-vitiligo-hold-back-article-1.1784516. Retrieved 9 May 2014.
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