Pigmentary Diseases PowerPoint Presentation PDF
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Duhok College of Medicine
Dr. Sarah Raed
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Summary
This presentation discusses pigmentary disorders, covering various causes, including albinism, piebaldism, and vitiligo. It also details management and treatment options. The presentation is likely part of a dermatology course.
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DISORDERS OF PIGMENTATION Dr. Sarah Raed Assistant Lecturer of Dermatology, Duhok.College of Medicine FITZPATRICK SKIN TYPES CLASSIFICATION SOME CAUSES OF HYPOPIGMENTATION OCULOCUTANEOUS ALBINISM Autosomal recessively inherited. There is a normal number of melan...
DISORDERS OF PIGMENTATION Dr. Sarah Raed Assistant Lecturer of Dermatology, Duhok.College of Medicine FITZPATRICK SKIN TYPES CLASSIFICATION SOME CAUSES OF HYPOPIGMENTATION OCULOCUTANEOUS ALBINISM Autosomal recessively inherited. There is a normal number of melanocytes in the basal layer of the epidermis, but lack tyrosinase and are unable to synthesize melanin. The whole skin is white and pigment is also lacking in the hair, iris and retina. Albinos have poor sight, photophobia and a nystagmus. Sunburn is common on unprotected skin. MANAGEMENT Albino patients must learn to protect themselves against UVR with sunscreens. Avoidance of sun wherever possible. Regular checking to detect early changes of skin cancer is also important. PIEBALDISM Autosomal dominant. Due to absence of melanocytes in the affected skin and hair follicles. In this condition, there is a white forelock and white patches on the skin surface PEIBALDISM VITILIGO Its an acquired, idiopathic disorder characterized by circumscribed Depigmented macules and patches Functional melanocytes disappear from involved skin by a mechanism(s) that has not yet been identified. EPIDEMIOLOGY Vitiligo occurs in 1–2% of the population. The disease affects both sexes equally. It may start at any age but usually affects children and young adults. It started before the age of 20 in 50% of the cases. PATHOGENESIS Multifactorial Genetic background is evident by presence of 30-40 % positive family history of vitiligo. The autoimmune hypothesis is the most acceptable theory. Inflammatory infiltrate consist mainly of T- lymphocytes, some of them invade the epidermis and destroy the melanocytes. CLINICAL FEATURES Sharply defined areas of depigmentation appear. The depigmented patches are often symmetrical, especially when they are over the limbs and face. It is a serious cosmetic problem for darkly pigmented people. The condition often starts in childhood and either spreads, ultimately causing total depigmentation, or persists, with irregular remissions and relapses. Vitiligo could be Generalized or Localized SYSTEMIC ASSOCIATION Increased risk of Autoimmune diseases: Thyroid dis. [Hashimoto’s, Grave’s] Addison’s disease Pernicious Anemia Insulin dependent Diabetes Alopecia Areata BAD PROGNOSTIC SIGNS: Very early onset in childhood. Lips and digits “Lip-tip vitiligo” Leukotrichia “Grey hair in the affected area”. Complete or universal type. Segmental type. Positive family history. WOOD’S LAMP TREATMENT Reassurance. Topical corticosteroids. Topical Immunomodulators such as tacrolimus, pimecrilamus. Photo(chemo)therapy:Narrow Band UVB (NBUVB) , Psoralen plus UVA (PUVA) TREATMENT Excimer Laser Sugrical :Minigrafting, Blister grafting, Cultured Autologous Melanocytes Cosmetic camouflage. Depigmentation : 20% monobenzyl ether of hydroquinone (MBEH) QUESTIONS ?