Human Inborn Errors of Immunity in Pyoderma Gangrenosum: A Systematic Review

IF 8.6 1区 医学 Q1 DERMATOLOGY
Yasmine Oprea, Daniel R. Antohi, Morgan Vague, Caroline Delbourgo Patton, Benedict Wu, Alex G. Ortega‐Loayza
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引用次数: 0

Abstract

Background and Objective

Pyoderma gangrenosum (PG) is a rare ulcerative neutrophilic dermatosis that can be associated with primary immunodeficiency. The pathogenesis of PG has not yet been elucidated, although contributions from dysregulation of the immune system in patients with apparent genetic predispositions have been postulated. We conducted a Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA)-guided systematic review with the objective of identifying inborn errors of immunity in the presence of PG as well as their clinical characteristics of severity including number of PG lesions and anatomic areas affected, and treatment outcomes.

Methods

A literature search was performed using PubMed/MEDLINE, Embase, Cochrane Library, and Web of Science through August 24, 2023, for studies published in English using the search terms: “pyoderma gangrenosum,” “inborn error of immunity,” “immune defect*,” and a list of genetic mutations potentially associated with PG.

Results

Seventy-four cases of PG associated with inborn errors of immunity were identified. The results demonstrate an association of PG with a variety of inborn errors of immunity, including genetic mutations not classically associated with the condition. Genetic mutations such as BTK, IL1RN, ITGB2, LPIN2, MEFV, NFkB1, NLRP3, NLRP12, NOD2, PSMB8, PLCG2, PSTPIP1, RAG1, TTC37, and WDR1, as well as complement component 2/complement component 4 (C2/C4) and complement component 7 (C7) deficiencies were identified in the presence of either idiopathic or syndromic PG. Of note, mutations in genes such as PSMB8, NLRP3, and IL1RN were found to be associated with a more severe and atypical course of PG, whereas mutations in RAG1 as well as those causing a C2/C4 deficiency were associated with the mildest clinical presentations of PG. Mutations in NFkB1, ITGB2, and PSTPIP1 were associated with the most heterogeneous clinical presentations.

Conclusions

Human inborn errors of immunity may be implicated in the genetic predisposition to PG and may influence the clinical presentation. Due to the rarity of these diseases, further work must be done to describe the association between inborn errors of immunity and PG. Identifying inborn errors of immunity that may contribute to the development of PG may assist in further elucidating the mechanism of PG, guiding targeted treatment, and improving clinical outcomes for these patients.

Abstract Image

脓皮病中的人类先天性免疫错误:系统综述
背景和目的:坏疽性脓皮病(PG)是一种罕见的溃疡性嗜中性皮肤病,可能与原发性免疫缺陷有关。尽管有人推测具有明显遗传倾向的患者的免疫系统失调可能是导致 PG 发病的原因之一,但 PG 的发病机制尚未阐明。我们在系统综述和荟萃分析首选报告项目(PRISMA)指导下进行了一次系统综述,目的是确定存在 PG 的先天性免疫错误及其严重程度的临床特征,包括 PG 病变的数量和受影响的解剖区域,以及治疗结果:方法:使用 PubMed/MEDLINE、Embase、Cochrane Library 和 Web of Science 对截至 2023 年 8 月 24 日以英文发表的研究进行文献检索,检索词包括"脓皮病"、"先天性免疫错误"、"免疫缺陷*"以及可能与 PG 相关的基因突变列表:结果:共发现 74 例与先天性免疫错误有关的脓疱疮病例。结果表明,PG 与多种先天性免疫错误有关,其中包括与该病症不相关的基因突变。在特发性或综合征 PG 中发现了 BTK、IL1RN、ITGB2、LPIN2、MEFV、NFkB1、NLRP3、NLRP12、NOD2、PSMB8、PLCG2、PSTPIP1、RAG1、TTC37 和 WDR1 等基因突变,以及补体成分 2/补体成分 4(C2/C4)和补体成分 7(C7)缺陷。值得注意的是,PSMB8、NLRP3 和 IL1RN 等基因的突变与 PG 更严重和不典型的病程有关,而 RAG1 基因突变以及导致 C2/C4 缺乏症的基因突变与 PG 最轻微的临床表现有关。NFkB1、ITGB2和PSTPIP1的突变与最异质性的临床表现有关:人类先天性免疫错误可能与 PG 的遗传易感性有关,并可能影响临床表现。结论:人类先天性免疫错误可能与 PG 的遗传易感性有关,并可能影响临床表现。由于此类疾病的罕见性,必须进一步研究先天性免疫错误与 PG 之间的关联。找出可能导致 PG 发病的先天性免疫错误可能有助于进一步阐明 PG 的发病机制、指导有针对性的治疗并改善这些患者的临床预后。
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来源期刊
CiteScore
15.20
自引率
2.70%
发文量
84
审稿时长
>12 weeks
期刊介绍: The American Journal of Clinical Dermatology is dedicated to evidence-based therapy and effective patient management in dermatology. It publishes critical review articles and clinically focused original research covering comprehensive aspects of dermatological conditions. The journal enhances visibility and educational value through features like Key Points summaries, plain language summaries, and various digital elements, ensuring accessibility and depth for a diverse readership.
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