A case of familial progressive hyperpigmentation with or without hypopigmentation presenting with hypopigmented striae along the lines of Blaschko

Tokimasa Hida, Masashi Idogawa, Aki Ishikawa, Masae Okura, Satoru Sasaki, Takashi Tokino, Hisashi Uhara
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Abstract

Familial progressive hyperpigmentation with or without hypopigmentation (FPHH) is an autosomal dominant disorder characterized by widespread skin hyperpigmentation, café‐au‐lait spots, and hypopigmented circular macules, resulting from KITLG variants. KITLG, expressed by keratinocytes, binds to KIT on melanocytes, stimulating melanogenesis. Disturbances in the KITLG‐KIT interaction result in diffuse hyperpigmentation in FPHH. However, the mechanisms behind hypopigmented macule formation remain unclear. This report presents a unique FPHH case in a patient with a novel KITLG mutation (Ser78Leu). Notably, the patient showed multiple hypopigmented macules and striae along the lines of Blaschko. Digital polymerase chain reaction analysis of the DNA from skin and blood tissues indicated a copy‐neutral loss of heterozygosity at the KITLG locus, only in the hypopigmented macule. These findings suggest that the hypopigmented macules might result from revertant mosaicism. Conversely, café‐au‐lait spots do not follow the lines of Blaschko and can superimpose on the hypopigmented striae, indicating a distinct pathogenesis. This case contributes to the understanding of the genetic mechanisms in FPHH.
一例伴有或不伴有色素减退的家族性进行性色素沉着症,表现为沿布拉什科纹的色素减退性条纹
家族性进行性色素沉着伴或不伴色素减退(FPHH)是一种常染色体显性遗传病,其特征是广泛的皮肤色素沉着、咖啡斑和色素减退性圆形斑丘疹,由 KITLG 变体引起。KITLG 由角质形成细胞表达,能与黑色素细胞上的 KIT 结合,刺激黑色素生成。KITLG-KIT 相互作用的紊乱会导致 FPHH 中弥漫性色素沉着。然而,色素沉着斑形成背后的机制仍不清楚。本报告介绍了一名患有新型 KITLG 突变(Ser78Leu)患者的独特 FPHH 病例。值得注意的是,该患者出现了多个色素减退性黄斑和沿布拉氏线的条纹。对来自皮肤和血液组织的 DNA 进行的数字聚合酶链反应分析表明,KITLG 基因座的杂合性缺失为拷贝中性,仅存在于色素减退斑中。这些发现表明,色素沉着斑可能是由回复嵌合引起的。相反,咖啡色斑并不遵循布拉什科线,而且可以叠加在色素减退斑上,这表明其发病机制不同。本病例有助于人们了解 FPHH 的遗传机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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