Abstract
The autoimmune basis of segmental vitiligo (SV) has only recently been recognized. Systemic autoimmune diseases are less frequently associated compared to non-segmental vitiligo (NSV), but localized skin disorders – in particular linear morphea – have been repeatedly observed in patients with SV. The inflammatory response is documented on a clinical level with cases displaying erythematous borders or a hypochromic stage, on a histopathological level with predominantly CD8 lymphocytes migrating toward the basal layer and by flow cytometry demonstrating the antimelanocyte specificity of these cytotoxic T cells. The increased risk for halo naevi and NSV in these patients further underline the immune-mediated mechanisms of SV. Nonetheless, the localized and unique distribution pattern points to somatic mosaicism. This places SV in a category of similar diseases such as lichen striatus, blaschkitis, linear lupus erythematosus, and linear scleroderma where an immune reaction against genetically mutated skin cells is believed to be the underlying cause. All these disorders are characterized by a young age of onset, a temporary disease activity with spontaneous resolution, limited response to treatment, and often long-term sequelae. Although challenging, genetic research proving this genetic mosaicism could offer crucial insights into the pathogenesis of both segmental and non-segmental vitiligo.
Highlights
The prevalence of vitiligo is reported to be around 0.5-1% of the population, remarkable regional differences exist [1]
Segmental vitiligo (SV) has several unique characteristics compared to non-segmental vitiligo (NSV)
Our group analyzed the lymphocytic infiltrate in a progressive case of SV more in-depth using HLA-peptide tetramers (MART-1, tyrosinase, gp100). We discovered both in lesional and nonlesional skin CD8 lymphocytes with a high production of IFN-g and TNF-a
Summary
Reinhart Speeckaert 1*, Jo Lambert 1, Vedrana Bulat 2, Arno Belpaire 1, Marijn Speeckaert 3 and Nanja van Geel 1. Systemic autoimmune diseases are less frequently associated compared to non-segmental vitiligo (NSV), but localized skin disorders – in particular linear morphea – have been repeatedly observed in patients with SV. The localized and unique distribution pattern points to somatic mosaicism This places SV in a category of similar diseases such as lichen striatus, blaschkitis, linear lupus erythematosus, and linear scleroderma where an immune reaction against genetically mutated skin cells is believed to be the underlying cause. All these disorders are characterized by a young age of onset, a temporary disease activity with spontaneous resolution, limited response to treatment, and often long-term sequelae.
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