Card14 功能获得性突变通过增强角质形成细胞对 IL-17A 的反应导致自发性银屑病样皮肤炎症。

Gain-of-Function Mutation of Card14 Leads to Spontaneous Psoriasis-like Skin Inflammation through Enhanced Keratinocyte Response to IL-17A.

机构信息

Institute for Immunology, Tsinghua University School of Medicine, Tsinghua University-Peking University Jointed Center for Life Sciences, Beijing, 100084, China.

Institute of Healthy Aging Research, Sun Yat-Sen University School of Life Sciences, Guangzhou, 510275, China.

出版信息

Immunity. 2018 Jul 17;49(1):66-79.e5. doi: 10.1016/j.immuni.2018.05.012. Epub 2018 Jul 3.

DOI:10.1016/j.immuni.2018.05.012

PMID:29980436

Abstract

Genetic mutations of CARD14 (encoding CARMA2) are observed in psoriasis patients. Here we showed that Card14 and Card14 mice developed spontaneous psoriasis-like skin inflammation, which resulted from constitutively activated CARMA2 via self-aggregation leading to the enhanced activation of the IL-23-IL-17A cytokine axis. Card14 mice displayed attenuated skin inflammation in the imiquimod-induced psoriasis model due to impaired IL-17A signaling in keratinocytes. CARMA2, mainly expressed in keratinocytes, associates with the ACT1-TRAF6 signaling complex and mediates IL-17A-induced NF-κB and MAPK signaling pathway activation, which leads to expression of pro-inflammatory factors. Thus, CARMA2 serves as a key mediator of IL-17A signaling and its constitutive activation in keratinocytes leads to the onset of psoriasis, which indicates an important role of NF-κB activation in keratinocytes in psoriatic initiation.

摘要

CARD14（编码 CARMA2）的基因突变在银屑病患者中观察到。在这里，我们表明 Card14 和 Card14 小鼠自发地发展出银屑病样皮肤炎症，这是由于自我聚集导致 CARMA2 的持续激活，从而增强了 IL-23-IL-17A 细胞因子轴的激活。Card14 小鼠在咪喹莫特诱导的银屑病模型中显示出皮肤炎症减弱，这是由于角质形成细胞中 IL-17A 信号受损所致。CARMA2 主要在角质形成细胞中表达，与 ACT1-TRAF6 信号复合物结合，并介导 IL-17A 诱导的 NF-κB 和 MAPK 信号通路激活，从而导致促炎因子的表达。因此，CARMA2 是 IL-17A 信号的关键介质，其在角质形成细胞中的组成性激活导致银屑病的发生，这表明 NF-κB 激活在银屑病发病机制中角质形成细胞中的重要作用。

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Card14 功能获得性突变通过增强角质形成细胞对 IL-17A 的反应导致自发性银屑病样皮肤炎症。

Gain-of-Function Mutation of Card14 Leads to Spontaneous Psoriasis-like Skin Inflammation through Enhanced Keratinocyte Response to IL-17A.

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