Characterization of the Pro-Inflammatory and Pruritogenic Transcriptome in Skin Lesions of the Experimental Canine Atopic Acute IgE-Mediated Late Phase Reactions Model and Correlation to Acute Skin Lesions of Human Atopic Dermatitis

A. Blubaugh, Kathleen Hoover, Sujung Jun Kim, Jonathan E. Fogle, Fatoumata Ba Sow, F. Banovic
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Abstract

Intradermal injection of anti-immunoglobulin E (IgE) antibodies in dogs grossly and histologically resemble naturally occurring atopic dermatitis (AD). However, the activated inflammatory and pruritic pathways have not been characterized. The objectives of this study were to characterize the inflammatory transcriptome of experimental acute canine IgE-induced lesions and to determine how these correlate to the transcriptome of naturally occurring human and canine acute atopic dermatitis. Biopsies were collected at 6 and 24 h after intradermal injections of anticanine-IgE antibodies to eight healthy male castrated Beagles; healthy and saline-injected skin served as controls. We extracted total RNA from skin biopsies and analyzed transcriptome using RNA-sequencing. Gene expressions of IgE-induced biopsies were compared to that of controls from the same subject (1.5-fold change, p-adjusted value ≤ 0.05). Acute IgE-mediated lesions had a significant upregulation of pro-inflammatory (e.g., LTB, IL-1B, PTX3, CCL2, IL6, IL8, IL18), T helper-(Th)1/IFNγ signal (e.g., STAT-1, OASL, MX-1, CXCL10, IL-12A) and Th2 (e.g., IL4R, IL5, IL13, IL33 and POSTN) genes, as well as Th2 chemokines (CCL17, CCL24). Pathway analysis revealed strong significant upregulation of JAK-STAT, histamine, IL-4 and IL13 signaling. Spearman correlation coefficient for the shared DEGs between canine anti-canine-IgE and human AD samples revealed a significant moderate positive correlation for anti-canine-IgE 6-h samples (r = 0.53) and 24-h samples (r = 0.47). In conclusion, acute canine IgE-mediated skin lesions exhibit a multipolar immunological axis upregulation (Th1, Th2 and Th17) in healthy dogs, resembling acute spontaneous human AD lesions.
实验性犬特应性急性 IgE 介导的晚期反应模型皮肤病变中促炎和致瘙痒转录组的特征以及与人类特应性皮炎急性皮肤病变的相关性
狗皮下注射抗免疫球蛋白 E(IgE)抗体在外观和组织学上与自然发生的特应性皮炎(AD)相似。然而,活化的炎症和瘙痒途径尚未定性。本研究的目的是描述实验性犬急性 IgE 诱导病变的炎症转录组,并确定这些转录组与自然发生的人类和犬急性特应性皮炎转录组的相关性。我们在 8 只健康雄性阉割比格犬皮内注射抗卡宁-IgE 抗体 6 小时和 24 小时后采集了活组织切片;健康皮肤和注射生理盐水的皮肤作为对照。我们从皮肤活检组织中提取了总 RNA,并使用 RNA 序列分析了转录组。将 IgE 诱导的活检组织的基因表达与同一受试者的对照组进行了比较(变化 1.5 倍,P 调整值 ≤ 0.05)。急性 IgE 介导的病变显著上调了促炎信号(如 LTB、IL-1B、PTX3、CCL2、IL6、IL8、IL18)、T 辅助细胞-(Th)1/IFNγ 信号(如 STAT-1、OASL、IFNγ)、T 辅助细胞-(Th)1/IFNγ 信号(如 STAT-1、OASL、IFNγ)、STAT-1、OASL、MX-1、CXCL10、IL-12A)和 Th2(如 IL4R、IL5、IL13、IL33 和 POSTN)基因,以及 Th2 趋化因子(CCL17、CCL24)。通路分析表明,JAK-STAT、组胺、IL-4 和 IL13 信号传导有明显的上调。犬抗犬IgE样本和人类AD样本之间共享DEGs的斯皮尔曼相关系数显示,抗犬IgE 6小时样本(r = 0.53)和24小时样本(r = 0.47)之间存在显著的中度正相关。总之,在健康犬中,IgE介导的急性犬皮肤病变表现出多极免疫轴上调(Th1、Th2和Th17),类似于急性自发性人类AD病变。
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