The Clinical and Molecular Response of Pyoderma Gangrenosum to Interleukin 23 Blockade: Result from a proof-of-concept open-label clinical trial.

Akshay Flora, James Pham, Jane A Woods, Michael Radzeika, Hugh Dickson, Mathew Malone, John W Frew
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Abstract

Pyoderma Gangrenosum is a severe ulcerative disease with a great need for novel therapies. A major barrier to the development of novel therapies is a lack of understanding of disease pathogenesis. We present the results of a proof-of-concept open label clinical trial of IL-23p19 antagonism with Tildrakizumab ion Pyoderma Gangrenosum. Gene expression analysis identified pro-inflammatory genes associated with interferon responses and dendritic cell activity including IFI27, XBP1, SAA1 LGALS3 and STAT3 significantly downregulated in lesional tissue after 12 weeks of therapy. Immunohistochemistry confirmed reduction in IL-17A and IL-17 F positive cells as well as reduction in TNF-a, C5a and IL-1B positive cells in week 12 samples compared to baseline. Significant reduction in serum inflammation was observed via serum proteomics, with IL-8, IL-6, and CASP-8 levels reduced comparable to healthy controls at Week 12. Clinical outcomes demonstrated significant reduction in ulcer size, pain, itch and quality of life outcomes in line with the molecular findings. Differential expression of key inflammatory cytokines such as IL-8, CXCL5, PD-L1, SPP1 and MMP1 were observed in tissue and serum when stratified by clinical responders and non-responders. This data provides insights into the clinical relevance of alterations in molecular markers in pyoderma gangrenosum and the potential for the identification of clinically relevant biomarkers of disease activity.

脓皮病对白细胞介素 23 阻断剂的临床和分子反应:概念验证开放标签临床试验的结果。
脓皮病是一种严重的溃疡性疾病,亟需新型疗法。开发新型疗法的主要障碍是缺乏对疾病发病机制的了解。我们介绍了用 Tildrakizumab 离子脓疱疮拮抗 IL-23p19 的开放标签临床试验的概念验证结果。基因表达分析确定了与干扰素反应和树突状细胞活性相关的促炎基因,包括 IFI27、XBP1、SAA1 LGALS3 和 STAT3,这些基因在治疗 12 周后的皮损组织中显著下调。免疫组化证实,与基线相比,第12周样本中IL-17A和IL-17 F阳性细胞减少,TNF-a、C5a和IL-1B阳性细胞减少。通过血清蛋白质组学观察到,血清中的炎症明显减少,第12周时,IL-8、IL-6和CASP-8水平的降低幅度与健康对照组相当。临床结果表明,溃疡面积、疼痛、瘙痒和生活质量均显著降低,与分子研究结果一致。根据临床应答者和非应答者进行分层,在组织和血清中观察到关键炎性细胞因子的差异表达,如 IL-8、CXCL5、PD-L1、SPP1 和 MMP1。这些数据有助于深入了解脓皮病分子标记物变化的临床相关性,以及确定疾病活动的临床相关生物标记物的潜力。
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