Dupilumab Therapy Modulates Circulating Inflammatory Mediators in Patients with Prurigo Nodularis

Aaron Bao , Emily Ma , Hannah Cornman , Anusha Kambala , Jaya Manjunath , Alexander L. Kollhoff , Brenda Umenita Imo , Madan M. Kwatra , Shawn G. Kwatra
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Abstract

Prurigo nodularis (PN) is a chronic inflammatory skin disease characterized by intense pruritus and skin nodules. Beyond the skin, PN involves circulating blood inflammation that may contribute to systemic disease comorbidities. Dupilumab was recently approved for treatment of PN, but its effects on systemic inflammation are unknown. Thus, we aimed to characterize changes in plasma concentrations of inflammatory proteins after dupilumab treatment. In this exploratory study, plasma samples were collected from 3 patients with moderate-to-severe PN before and after ≥6 months of dupilumab treatment. All patients exhibited clinically significant improvements after treatment. Of the 2569 proteins tested, 186 were differentially expressed after treatment (q < 0.1, fold change > 1.3). Downregulated proteins included cytokines associated with T helper (Th) 1 (IFN-γ, TNF-α), Th2 (IL-4, IL-13), and Th17/Th22 (IL-6, IL-22) signaling. Markers of innate immunity (IL-19, toll-like receptor 1, nitric oxide synthase 2), immune cell migration (CCL20, CD177), and fibrosis (IL-11, IL-22) were also decreased (q < 0.1). Gene set variation analysis of Th2, Th17, and epithelial–mesenchymal transition gene sets showed reduced pathway expression in the post-treatment cohort (P < .05). Plasma cytokine levels of IL-11, nitric oxide synthase 2, IL-13, IL-4, and IFNG (R2 > 0.75, q < 0.10) showed the strongest correlations with pruritus severity. Dupilumab may reduce systemic inflammatory proteins associated with multiple immune and fibrosis pathways in patients with PN, potentially modulating the development of systemic disease comorbidities.

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杜匹单抗疗法可调节结节性瘙痒症患者体内的循环炎症介质
结节性瘙痒症(PN)是一种慢性炎症性皮肤病,以剧烈瘙痒和皮肤结节为特征。除皮肤外,PN 还涉及血液循环炎症,可能导致全身性疾病合并症。杜匹单抗最近被批准用于治疗 PN,但其对全身炎症的影响尚不清楚。因此,我们的目的是描述杜匹单抗治疗后血浆中炎症蛋白浓度的变化。在这项探索性研究中,我们收集了 3 位中度至重度 PN 患者在接受≥6 个月的杜匹单抗治疗前后的血浆样本。治疗后,所有患者的临床症状均有明显改善。在检测的 2569 个蛋白质中,有 186 个在治疗后有差异表达(q < 0.1,折叠变化 > 1.3)。下调的蛋白质包括与T辅助(Th)1(IFN-γ、TNF-α)、Th2(IL-4、IL-13)和Th17/Th22(IL-6、IL-22)信号传导相关的细胞因子。先天性免疫标记物(IL-19、toll 样受体 1、一氧化氮合酶 2)、免疫细胞迁移(CCL20、CD177)和纤维化(IL-11、IL-22)也有所下降(q < 0.1)。Th2、Th17和上皮-间质转化基因组的基因组变异分析表明,治疗后队列中的通路表达减少(P <.05)。血浆细胞因子 IL-11、一氧化氮合酶 2、IL-13、IL-4 和 IFNG 的水平(R2 > 0.75,q < 0.10)与瘙痒严重程度的相关性最强。杜匹鲁单抗可减少PN患者与多种免疫和纤维化途径相关的全身炎症蛋白,从而有可能调节全身性疾病合并症的发展。
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CiteScore
4.00
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审稿时长
8 weeks
期刊最新文献
Cover 1 Corrigendum to ‘Proteomic Profiling of CCCA Reveals Role of Humoral Immune Response Pathway and Metabolic Dysregulation’ JID Innovations, Volume 4, Issue 3, May 2024, 100263 Identification of Associations with Dermatologic Diseases through a Focused GWAS of the UK Biobank From Plant to Patient: A Historical Perspective and Review of Selected Medicinal Plants in Dermatology Spatial Transcriptomics in Inflammatory Skin Diseases Using GeoMx Digital Spatial Profiling: A Practical Guide for Applications in Dermatology
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