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特定遗传背景下的自身炎症性皮肤表现的命名。

Designation of Autoinflammatory Skin Manifestations With Specific Genetic Backgrounds.

机构信息

Department of Dermatology, Wakayama Medical University, Wakayama, Japan.

出版信息

Front Immunol. 2020 Mar 18;11:475. doi: 10.3389/fimmu.2020.00475. eCollection 2020.

Abstract

"Autoinflammatory disease (AiD)" has first been introduced in 1999 when the responsible gene for the familial Hibernean fever or autosomal dominant-type familial Mediterranean fever-like periodic fever syndrome was reportedly identified as . Linked with the rapid research progress in the field of innate immunity, "autoinflammation" has been designated for dysregulated innate immunity in contrast to "autoimmunity" with dysregulated acquired immunity. As hereditary periodic fever syndromes represent the prototype of AiD, monogenic systemic diseases are the main members of AiD. However, skin manifestations provide important clinical information and there are even some AiDs originating from skin diseases. Recently, AiD showing psoriasis and related keratinization diseases have specifically been designated as "autoinflammatory keratinization diseases (AiKD)" and CARD14-associated psoriasis and deficiency of interleukin-36 receptor antagonist previously called as generalized pustular psoriasis are included. Similarly, a number of autoinflammatory skin diseases can be proposed; autoinflamatory urticarial dermatosis (AiUD) such as cryopyrin-associated periodic syndrome; autoinflammatory neutrophilic dermatosis (AiND) such as pyogenic sterile arthritis, pyoderma gangrenosm, and acne syndrome; autoinflammatory granulomatosis (AiG) such as Blau syndrome; autoinflammatory chilblain lupus (AiCL) such as Aicardi-Goutieres syndrome; autoinflammatory lipoatrophy (AiL) such as Nakajo-Nishimura syndrome; autoinflammatory angioedema (AiAE) such as hereditary angioedema; and probable autoinflammatory bullous disease (AiBD) such as granular C3 dermatosis. With these designations, skin manifestations in AiD can easily be recognized and, even more importantly, autoinflammatory pathogenesis of common skin diseases are expected to be more comprehensive.

摘要

"自身炎症性疾病(Autoinflammatory disease,AiD)" 一词于 1999 年首次提出,当时报道称家族性周期性发热或常染色体显性家族性地中海热样周期性发热综合征的致病基因已被鉴定为 。与先天免疫领域的快速研究进展相关联,"自身炎症" 被指定为先天免疫失调,而 "自身免疫" 则为获得性免疫失调。由于遗传性周期性发热综合征是 AiD 的原型,单基因系统性疾病是 AiD 的主要成员。然而,皮肤表现提供了重要的临床信息,甚至有些 AiD 起源于皮肤病。最近,表现为银屑病和相关角化病的 AiD 被特别指定为 "自身炎症性角化病(Autoinflammatory keratinization diseases,AiKD)",以前称为全身性脓疱性银屑病的 CARD14 相关银屑病和白细胞介素-36 受体拮抗剂缺乏症也包括在内。同样,可以提出许多自身炎症性皮肤病;如 Cryopyrin 相关周期性综合征的自身炎症性荨麻疹性皮肤病(Autoinflammatory urticarial dermatosis,AiUD);如化脓性关节炎、坏疽性脓皮病和痤疮综合征的自身炎症性中性粒细胞皮肤病(Autoinflammatory neutrophilic dermatosis,AiND);如 Blau 综合征的自身炎症性肉芽肿病(Autoinflammatory granulomatosis,AiG);如 Aicardi-Goutieres 综合征的自身炎症性冻疮样狼疮(Autoinflammatory chilblain lupus,AiCL);如 Nakajo-Nishimura 综合征的自身炎症性脂肪萎缩(Autoinflammatory lipoatrophy,AiL);如遗传性血管性水肿的自身炎症性血管性水肿(Autoinflammatory angioedema,AiAE);以及如颗粒性 C3 皮肤病的可能自身炎症性大疱病(Autoinflammatory bullous disease,AiBD)。有了这些命名,AiD 的皮肤表现很容易被识别,更重要的是,常见皮肤病的自身炎症发病机制有望更加全面。

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