A case of peeling skin syndrome type 1 with novel CDSN gene variation successfully treated with upadacitinib.

Yusha Chen, Jia Geng, Yue Xiao, Xingli Zhou, Mengmeng Li, Wei Li
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Abstract

Peeling skin syndrome type 1 (PSS1) is an autosomal recessive genodermatosis caused by the CDSN gene loss-of-function mutation and characterized by widespread superficial skin peeling and erythroderma with unbearable pruritus. Because of its ultra-rarity and unclear mechanism, this rare disease has no established treatment regimen. Herein, we reported a Chinese woman who presented with congenital generalized pruritic erythroderma and exfoliation, notable for significantly elevated IgE levels. The whole exome sequencing identified an unpublished homozygous variant (c.295C>T, p.Gln99*) in the CDSN gene, confirming the diagnosis of PSS1. Immunohistochemistry analysis of the affected skin confirmed the lack of corneodesmosin expression, revealed the overexpression of T helper 2 (Th2)-related cytokines harboring interleukin (IL) 4 and IL-13. After Janus kinase 1 (JAK1) inhibitor upadacitinib administration, both the patient's skin rashes and itching symptoms were significantly alleviated. Our work expanded the PSS1-related CDSN gene mutation spectrums, substantiated the hypothesis regarding the overexpression of Th2-related cytokines, and uncovered the important role of JAK1 underlying PSS1. JAK1 signaling may dominate the pathogenesis in PSS1 and represent a potential therapeutic target.

一例伴有新型 CDSN 基因变异的 1 型脱皮综合征患者成功接受了达达替尼治疗。
1 型剥脱性皮肤综合征(PSS1)是一种常染色体隐性遗传性皮肤病,由 CDSN 基因功能缺失突变引起,以广泛的表皮剥脱和红斑伴难以忍受的瘙痒为特征。由于这种罕见病极为罕见,发病机制不清,目前尚无成熟的治疗方案。在此,我们报告了一名先天性全身瘙痒性红斑和脱皮的中国女性患者,她的显著特点是 IgE 水平明显升高。全外显子组测序发现了 CDSN 基因中一个未公开的同源变异(c.295C>T, p.Gln99*),确诊为 PSS1。受影响皮肤的免疫组化分析证实缺乏角化棘球蛋白表达,并发现白细胞介素(IL)4和IL-13等与T辅助细胞2(Th2)相关的细胞因子过度表达。在服用 Janus 激酶 1(JAK1)抑制剂乌达替尼后,患者的皮疹和瘙痒症状均明显缓解。我们的研究拓展了与PSS1相关的CDSN基因突变谱,证实了Th2相关细胞因子过度表达的假说,并揭示了JAK1在PSS1中的重要作用。JAK1 信号转导可能主导 PSS1 的发病机制,是潜在的治疗靶点。
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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