Aryl hydrocarbon receptor and IL-13 signaling crosstalk in human keratinocytes and atopic dermatitis

IF 3.3 Q2 ALLERGY Frontiers in allergy Pub Date : 2024-01-26 DOI:10.3389/falgy.2024.1323405
S. Proper, Alexander T. Dwyer, Andrews Appiagyei, J. Felton, Netali Ben-Baruch Morgenstern, Justin M. Marlman, M. Kotliar, Artem Barski, Ty D. Troutman, Marc E. Rothenberg, T. Mersha, N. Azouz
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Abstract

Atopic dermatitis (AD) is an allergic skin disease mediated by skin barrier impairment and IL-13-driven immune response. Activation of the aryl hydrocarbon receptor (AHR) has shown promise in early clinical trials for AD; however, the mechanism by which AHR partially ameliorates AD is not well known.Gene expression data from human biopsies were analyzed, and compared to gene expression from RNA-sequencing in our in-vitro HaCaT cell model system. Western blot, ELISA qRT-PCR were used to further explore the relationship between AHR and IL-13 signaling in HaCaT cells.The AHR target gene CYP1A1 was decreased in lesional skin compared with healthy control skin (p = 4.30 × 10−9). Single-cell RNA sequencing (scRNAseq) demonstrated increased AHR expression (p < 1.0 × 10−4) and decreased CYP1A1 expression in lesional AD keratinocytes compared with healthy control keratinocytes (p < 0.001). Activation of AHR by AHR agonists in HaCaT cells reversed IL-13-dependent gene expression of several key genes in AD pathogenesis, most notably the eosinophil chemoattractant CCL26 (eotaxin-3). Differentially expressed genes in keratinocytes of patients with AD substantially overlapped with genes regulated by AHR agonists from HaCaT cells by RNAseq, but in reverse direction. Mechanistically, there was evidence for direct transcriptional effects of AHR; AHR binding motifs were identified in the differentially expressed genes from lesional AD keratinocytes compared to control keratinocytes, and AHR activation did not modify IL-13-dependent signal transducer and activator of transcription 6 (STAT6) translocation to the nucleus.Together, these data suggest that the AHR pathway is dysregulated in AD and that AHR modulates IL-13 downstream signaling in keratinocytes through genome-wide, transcriptional regulatory effects.
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人类角质细胞和特应性皮炎中芳基烃受体和 IL-13 信号的相互影响
特应性皮炎(AD)是一种由皮肤屏障受损和 IL-13 驱动的免疫反应介导的过敏性皮肤病。我们分析了人体活检组织的基因表达数据,并将其与体外 HaCaT 细胞模型系统中 RNA 测序的基因表达进行了比较。通过 Western blot、ELISA qRT-PCR,进一步探讨了 HaCaT 细胞中 AHR 和 IL-13 信号转导之间的关系。与健康对照皮肤相比,病变皮肤中 AHR 靶基因 CYP1A1 的表达量有所下降(p = 4.30 × 10-9)。单细胞 RNA 测序(scRNAseq)显示,与健康对照组角质细胞相比,AD 病变角质细胞中 AHR 表达增加(p < 1.0 × 10-4),CYP1A1 表达减少(p < 0.001)。在 HaCaT 细胞中用 AHR 激动剂激活 AHR 可逆转 AD 发病机制中几个关键基因的 IL-13 依赖性基因表达,其中最显著的是嗜酸性粒细胞趋化吸引剂 CCL26(eotaxin-3)。通过RNAseq分析,AD患者角质细胞中的差异表达基因与HaCaT细胞中受AHR激动剂调控的基因有很大程度的重叠,但方向相反。从机理上讲,有证据表明AHR具有直接转录效应;与对照组角朊细胞相比,病变AD角朊细胞的差异表达基因中发现了AHR结合基序,而AHR激活并不改变依赖于IL-13的信号转导子和转录激活子6(STAT6)向细胞核的转位。这些数据共同表明,AHR通路在AD中失调,AHR通过全基因组转录调控效应调节角朊细胞中的IL-13下游信号转导。
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2.80
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0.00%
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审稿时长
12 weeks
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