特应性皮炎 IFNG 高表达亚群和低表达亚群的特征

S. Wasserer, M. Jargosch, K. E. Mayer, Jessica Eigemann, Theresa Raunegger, Görkem Aydin, S. Eyerich, T. Biedermann, K. Eyerich, Felix Lauffer
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引用次数: 0

摘要

特应性皮炎(AD)是最常见的慢性炎症性皮肤病之一,目前有越来越多的靶向疗法可供选择。治疗特应性皮炎的生物制剂只针对 2 型免疫的关键细胞因子,而 Janus 激酶抑制剂则针对包括 IFN-γ 在内的多种细胞因子。由于IFNG在AD中的作用尚未完全明确,为了更好地对患者进行分层以获得最佳治疗效果,亚组的识别和特征描述(尤其是IFNG的表达)具有重要意义。本研究旨在根据病变 IFNG 的表达界定 AD 亚组,并根据基因表达、T 细胞分泌组和临床特征对亚组进行特征描述。研究人员通过 RNA 测序分析了 48 例 AD 患者病变和非病变活检组织的 RNA。根据病变T细胞的IFNG基因表达和IFN-γ的释放情况,采用无监督聚类方法将这批患者分为三个IFNG组(高、中、低)。低IFNG组显示了外源性AD的特征,特应性合并症和表皮脂质合成受损的发病率较高。相比之下,高IFNG组患者的平均年龄较高,并激活了其他促炎途径。在细胞水平上,通过去卷积算法,高IFNG组比低IFNG组检测到更多的M1巨噬细胞和自然杀伤细胞信号。不过,两组都有一个共同的杜匹单抗反应基因特征,表明在两个亚组中,2型免疫是主要的免疫转变。总之,高IFNG亚组和低IFNG亚组对应于AD的内在和外在分类,将来可用于评估疗效或无应答者。
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Characterization of High and Low IFNG-Expressing Subgroups in Atopic Dermatitis
Atopic dermatitis (AD) is one of the most common chronic inflammatory skin diseases, with an increasing number of targeted therapies available. While biologics to treat AD exclusively target the key cytokines of type 2 immunity, Janus kinase inhibitors target a broad variety of cytokines, including IFN-γ. To better stratify patients for optimal treatment outcomes, the identification and characterization of subgroups, especially with regard to their IFNG expression, is of great relevance, as the role of IFNG in AD has not yet been fully clarified. This study aims to define AD subgroups based on their lesional IFNG expression and to characterize them based on their gene expression, T cell secretome and clinical attributes. RNA from the lesional and non-lesional biopsies of 48 AD patients was analyzed by RNA sequencing. Based on IFNG gene expression and the release of IFN-γ by lesional T cells, this cohort was categorized into three IFNG groups (high, medium, and low) using unsupervised clustering. The low IFNG group showed features of extrinsic AD with a higher prevalence of atopic comorbidities and impaired epidermal lipid synthesis. In contrast, patients in the high IFNG group had a higher average age and an activation of additional pro-inflammatory pathways. On the cellular level, higher amounts of M1 macrophages and natural killer cell signaling were detected in the high IFNG group compared to the low IFNG group by a deconvolution algorithm. However, both groups shared a common dupilumab response gene signature, indicating that type 2 immunity is the dominant immune shift in both subgroups. In summary, high and low IFNG subgroups correspond to intrinsic and extrinsic AD classifications and might be considered in the future for evaluating therapeutic efficacy or non-responders.
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