UBE2N 对维持皮肤稳态和抑制炎症至关重要。

The Journal of investigative dermatology Pub Date : 2024-12-01 Epub Date: 2024-05-23 DOI:10.1016/j.jid.2024.04.017
Min Jin Lee, Manel Ben Hammouda, Wanying Miao, Arinze E Okafor, Yingai J Jin, Huiying Sun, Vaibhav Jain, Vadim Markovtsov, Yarui Diao, Simon G Gregory, Jennifer Y Zhang
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引用次数: 0

摘要

UBE2N是一种Lys63-泛素连接酶,在胚胎发生和免疫系统的发育与功能中发挥着关键作用。然而,它在成人上皮组织稳态和发病机制中的作用尚不清楚。我们生成了条件性小鼠模型,以时间和空间控制的方式在皮肤细胞中删除了 Ube2n。我们发现,成年皮肤角质细胞中的 Ube2n 基因敲除(KO)会诱发一系列具有银屑病和日光性角化病特征的炎症性皮肤缺陷。这些缺陷包括炎症、表皮和真皮增厚、角化不全、免疫细胞浸润增加以及水肿和水疱症状。单细胞转录组分析和 RT-qPCR 显示,Ube2n KO 的角朊细胞表达了升高的髓细胞趋化吸引因子,如 Cxcl1 和 Cxcl2,并减少了同源 T 淋巴细胞趋化吸引因子 Ccl27a。同样,浸润的免疫细胞主要是髓源性细胞,包括中性粒细胞和 M1 样巨噬细胞,它们表达高水平的炎性细胞因子,如 Il1β 和 Il24。药物阻断 IL-1 受体相关激酶(IRAK1/4)可减轻 Ube2n 突变体皮肤的炎症、表皮和真皮增厚以及免疫浸润。总之,这些发现突出了角质形成细胞-UBE2N在维持表皮稳态和皮肤免疫中的关键作用,并确定IRAK1/4是炎症性皮肤病的潜在治疗靶点。
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UBE2N Is Essential for Maintenance of Skin Homeostasis and Suppression of Inflammation.

UBE2N, a Lys63 ubiquitin-conjugating enzyme, plays critical roles in embryogenesis and immune system development and function. However, its roles in adult epithelial tissue homeostasis and pathogenesis are unclear. We generated conditional mouse models that deleted Ube2n in skin cells in a temporally and spatially controlled manner. We found that Ube2n knockout in the adult skin keratinocytes induced a range of inflammatory skin defects characteristic of psoriatic and actinic keratosis. These included inflammation, epidermal and dermal thickening, parakeratosis, and increased immune cell infiltration as well as signs of edema and blistering. Single-cell transcriptomic analyses and RT-qPCR showed that Ube2n-knockout keratinocytes expressed elevated myeloid cell chemoattractants such as Cxcl1 and Cxcl2 and decreased the homeostatic T lymphocyte chemoattractant Ccl27a. Consistently, the infiltrating immune cells were predominantly myeloid-derived cells, including neutrophils and M1-like macrophages, which expressed high levels of inflammatory cytokines such as Il1β and Il24. Pharmacological blockade of the IL-1 receptor associated kinases (IRAK1/4) alleviated inflammation, epidermal and dermal thickening, and immune infiltration of the Ube2n-mutant skin. Together, these findings highlight a key role of keratinocyte UBE2N in maintenance of epidermal homeostasis and skin immunity and identify IRAK1/4 as potential therapeutic target for inflammatory skin disorders.

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