胶原蛋白 XXIII alpha 1 的鉴定和特征描述--它是疱疹性湿疹的新型风险因素

medRxiv - Dermatology Pub Date : 2024-07-14 DOI:10.1101/2024.07.13.24310236

Shruti Chopra, Lennart M. Roesner, Katinka Döhner, Jana Zeitvogel, Stephan Traidl, Elke Rodriguez, Inken Harder, Lieb Wolfgang, Stephan Weidinger, Thomas F. Schulz, Beate Sodeik, Thomas Werfel

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引用次数: 0

摘要

摘要背景：特应性皮炎（AD）患者中有一个亚群容易感染单纯疱疹病毒（HSV），出现严重的播散性皮肤感染，即带状疱疹湿疹（EH）。EH发生在一部分AD患者中，而且经常复发，这意味着遗传因素在其发病机制中的重要性。目的：我们旨在确定EH的新型遗传风险因素，并研究其对HSV-1感染的影响。方法：我们对9名有（ADEH+）和无（ADEH-）EH病史的AD患者进行了全外显子组测序，并与健康对照组进行了比较。我们通过PCR方法在117名ADEH+、117名ADEH-患者和118名健康对照者中验证了ADEH中COL23A1基因（编码XXIII型胶原蛋白α1链）变异的发现。我们研究了 COL23A1 在 ADEH+ 和 ADEH- 患者角质细胞中的表达，以及 COL23A1 在原发性角质细胞和细胞系 HaCaT 中的上调表达，以研究其在 HSV-1 感染中的作用。结果：我们在5%的ADEH+患者、1.6%的健康供体和0%的ADEH-患者中发现了COL23A1中的单核苷酸多态性（SNP）rs2973744，它是EH的一个风险因素。与 ADEH- 患者的角朊细胞相比，带有 SNP rs2973744 的 ADEH+ 患者的原代人类角朊细胞表达更高的 COL23A1 水平，对 HSV-1 更易感。在功能测试中，我们发现在 COL23A1 表达量增加的角质细胞中，HSV-1 基因表达和细胞间传播的效率更高。此外，COL23A1在HaCaT细胞中的过表达导致参与有效免疫反应的多个基因（IL1R1、IL32、TLR4、CFH、C3、S100A9、IRF1和ADAM23）转录下调，而与AD相关的TNC和SPINK5则显著上调。结论：COL23A1的上调可能通过削弱角朊细胞的抗病毒反应来促进HSV-1感染。在其他标记中，COL23A1 SNP rs2973744可用于AD患者的筛查，以识别有EH风险的患者，从而及早开始治疗。

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Identification and characterization of collagen XXIII alpha 1 as a novel risk factor for eczema herpeticum

Abstract Background: A subgroup of atopic dermatitis (AD) patients is prone to develop severe, disseminated cutaneous infection with herpes simplex virus (HSV), known as eczema herpeticum (EH). The occurrence of EH in a subset of AD patients and its frequent recurrence implies the importance of genetic factors in its pathogenesis. Objective: We aimed to identify novel genetic risk factors for EH and study their impact on HSV-1 infection. Methods: We performed whole exome sequencing on nine AD patients with (ADEH+) and without (ADEH-) a history of EH in comparison to healthy controls. We validated the finding of a variant of COL23A1 gene (encoding Collagen type XXIII alpha 1 chain) in ADEH in a larger cohort of 117 ADEH+, 117 ADEH- patients and 118 healthy controls by PCR. We studied the expression of COL23A1 in keratinocytes from ADEH+ and ADEH- patients, and the upregulated COL23A1 expression in primary keratinocytes and in the cell line HaCaT to study its role in HSV-1 infection. Results: We identified a single nucleotide polymorphism (SNP), rs2973744 in COL23A1, as a risk factor for EH observed in 5% of ADEH+ patients, 1.6% of healthy donors and 0% of ADEH- patients. Primary human keratinocytes from an ADEH+ patient with SNP rs2973744 expressed higher COL23A1 levels and were more susceptible to HSV-1 than keratinocytes from ADEH- patients. In functional assays we showed that HSV-1 gene expression and cell-to-cell spread was more efficient in keratinocytes with increased expression of COL23A1. Moreover, COL23A1 overexpression in HaCaT cells resulted in transcriptional downregulation of several genes that are involved in an effective immune response (IL1R1, IL32, TLR4, CFH, C3, S100A9, IRF1, and ADAM23) and a notable upregulation of TNC and SPINK5 that are associated with AD. Conclusion: Upregulation of COL23A1 promotes HSV-1 infection presumably by attenuating antiviral responses of keratinocytes. Among other markers, the COL23A1 SNP rs2973744 could be included in the screening of AD patients to identify patients at risk of EH, thus allowing early initiation of therapy.

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medRxiv - Dermatology

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