A case of revertant mosaic-like normal-looking spots in a patient with erythroderma with IL36RN and CARD14 heterozygous mutations.

The Journal of dermatology Pub Date : 2024-10-07 DOI:10.1111/1346-8138.17498

Maho Matsuo, Xiaoyu Zang, Toshinari Miyauchi, Yoko Mizutani, Hirofumi Niwa, Kayoko Tanaka, Hiroaki Iwata

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Abstract

An 89-year-old Japanese woman presented with erythroderma associated with significant scaling. A histological examination showed acanthosis with hyperkeratosis and hyperkeratinization of the hair follicles. Genetic analyses using DNA from the peripheral blood revealed heterozygous mutations in IL36RN (c.115+6T>C) and CARD14 c.2648G>A (p.Arg883His). Based on these findings, we diagnosed her with erythroderma attributable to autoinflammatory keratinization disease. She then developed more than 30 small, round, well-defined, spots on her back and extremities that appeared histologically normal. We suspected that these spots might be revertant mosaicism. Immunohistochemical staining with p65, which is a component of nuclear factor kappa-light-chain-enhancer of activated B cells (NF-kB), revealed nuclear staining in epidermal keratinocytes in erythematous lesions, but not in the normal-looking spots. However, mutations in IL36RN and CARD14 unexpectedly persisted in the epidermis and dermis of the normal-looking spots.

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一例因 IL36RN 和 CARD14 基因杂合突变而患红斑狼疮的患者身上出现了马赛克样正常外观的还原斑。

一名 89 岁的日本妇女出现红斑，伴有明显脱屑。组织学检查显示毛囊角化过度和过度角质化。利用外周血 DNA 进行的基因分析表明，IL36RN（c.115+6T>C）和 CARD14 c.2648G>A （p.Arg883His）存在杂合突变。根据这些结果，我们诊断她患有自身炎症性角化病引起的红皮病。随后，她的背部和四肢出现了 30 多个圆形、轮廓清晰的小斑点，组织学上看起来正常。我们怀疑这些斑点可能是返祖嵌合。用 p65（活化 B 细胞的核因子卡巴轻链增强因子（NF-kB）的一种成分）进行免疫组化染色，发现红斑病灶中的表皮角质细胞有核染色，而外观正常的斑点中却没有。然而，IL36RN 和 CARD14 的突变却意外地在外观正常的斑点的表皮和真皮中持续存在。

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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The Journal of dermatology

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