Centre for Dermatology Research, Northern Care Alliance NHS Foundation Trust, The University of Manchester, Manchester Academic Health Science Centre, NIHR Manchester Biomedical Research Centre, Manchester, United Kingdom.
Centre for Genetics and Genomics Versus Arthritis, Centre for Musculoskeletal Research, University of Manchester, Manchester, United Kingdom; The Lydia Becker Institute of Immunology and Inflammation, Faculty of Biology, Medicine and Health, University of Manchester, Manchester, United Kingdom.
J Allergy Clin Immunol. 2023 Nov;152(5):1237-1246. doi: 10.1016/j.jaci.2023.07.011. Epub 2023 Aug 1.
Few studies have explored the immunology and genetic risk of paradoxical eczema occurring as an adverse event of biologic therapy in patients with psoriasis.
We sought to describe the systemic inflammatory signature of paradoxical eczema using proteomics and explore whether this is genetically mediated.
This study used the Olink Target 96 Inflammation panel on 256 serum samples from 71 patients with psoriasis and paradoxical eczema, and 75 controls with psoriasis to identify differentially expressed proteins and enriched gene sets. Case samples from 1 or more time points (T1 prebiologic, T2 postbiologic, and T3 postparadoxical eczema) were matched 1:1 with control samples. Genes contributing to enriched gene sets were selected, and functional single nucleotide polymorphisms used to create polygenic risk scores in a genotyped cohort of 88 paradoxical eczema cases and 3124 psoriasis controls.
STAMBP expression was lower in cases at T1 than in controls (log-fold change: -0.44; adjusted P = .022); no other proteins reached statistical significance at equivalent time points. Eleven gene sets including cytokine and chemokine pathways were enriched in cases at T2 and 10 at T3. Of the 39 proteins contributing to enriched gene sets, the majority are associated with the atopic dermatitis serum proteome. A polygenic risk score including 38 functional single nucleotide polymorphisms linked to enriched gene sets was associated with paradoxical eczema (adjusted P = .046).
The paradoxical eczema systemic inflammatory proteome trends toward atopic dermatitis at a gene-set level and is detectable before onset of the phenotype. This signature could be genetically determined.
鲜有研究探讨银屑病患者接受生物治疗后出现的矛盾性湿疹的免疫学和遗传风险。
我们旨在通过蛋白质组学描述矛盾性湿疹的系统性炎症特征,并探讨其是否具有遗传介导性。
本研究使用 Olink Target 96 炎症面板,对 71 例银屑病和矛盾性湿疹患者(病例组)及 75 例银屑病对照(对照组)的 256 份血清样本进行检测,以鉴定差异表达蛋白和富集基因集。对来自 1 个或多个时间点(T1 生物治疗前、T2 生物治疗后、T3 矛盾性湿疹后)的病例样本进行 1:1 匹配对照样本。选择对富集基因集有贡献的基因,并在一个经基因分型的 88 例矛盾性湿疹病例和 3124 例银屑病对照的队列中,使用功能性单核苷酸多态性构建多基因风险评分。
与对照组相比,病例组 T1 时的 STAMBP 表达较低(对数倍变化:-0.44;调整 P =.022);在其他等效时间点无其他蛋白达到统计学意义。T2 时有 11 个基因集包括细胞因子和趋化因子途径,T3 时有 10 个基因集。在对富集基因集有贡献的 39 种蛋白中,大多数与特应性皮炎的血清蛋白质组相关。一个包含 38 个与富集基因集相关的功能性单核苷酸多态性的多基因风险评分与矛盾性湿疹相关(调整 P =.046)。
矛盾性湿疹的系统性炎症蛋白质组在基因集水平上呈特应性皮炎趋势,在表型出现之前即可检测到。该特征可能具有遗传决定。
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