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未来化脓性汗腺炎治疗的靶分子。

Target molecules for future hidradenitis suppurativa treatment.

作者信息

Zouboulis Christos C, Frew John W, Giamarellos-Bourboulis Evangelos J, Jemec Gregor B E, Del Marmol Veronique, Marzano Angelo V, Nikolakis Georgios, Sayed Christopher J, Tzellos Thrasyvoulos, Wolk Kerstin, Prens Errol P

机构信息

European Hidradenitis Suppurativa Foundation e.V., Dessau, Germany.

Departments of Dermatology, Venereology, Allergology and Immunology, Dessau Medical Center, Brandenburg Medical School Theodor Fontane and Faculty of Health Sciences Brandenburg, Dessau, Germany.

出版信息

Exp Dermatol. 2021 Jun;30 Suppl 1:8-17. doi: 10.1111/exd.14338.

DOI:10.1111/exd.14338
PMID:34085329
Abstract

The registration of the tumour necrosis factor-α inhibitor adalimumab in 2015 was a major step forward in the treatment of hidradenitis suppurativa/acne inversa (HS). However, it soon became evident that the effectiveness of adalimumab in daily practice was highly variable. A significant unmet medical need of HS patients remained, and the search for novel therapeutic targets was intensified. During the 10th European Hidradenitis Suppurativa Foundation (EHSF) e.V. Conference, reknown international HS investigators virtually presented and discussed the published data on these potential target molecules for future HS treatment. This article addresses the most promising molecules currently under investigation from a pathophysiological and clinical point of view. With phase III trials ongoing, the anti- interleukin (IL)-17 biologics bimekizumab and secukinumab are in the most advanced stage of clinical development showing promising results. In addition, targeting IL-1α with bermekimab has shown encouraging results in two clinical trials. Directing treatment at neutrophil recruitment and activation by targeting IL-36 with spesolimab fits well in the pathogenic concept of HS and clinical phase II trial results are pending. In contrast to in situ evidence, Complement 5a (C5a) and C5a receptor blockade have only shown greater clinical benefit in patients with severe HS. Inhibition of Janus kinase (JAK) 1 signalling in HS showed clinical efficacy only in the highest dosage, highlighting that careful surveillance of the balance between safety and efficacy of JAK inhibition is warranted. Overall, clinical efficacies of all novel treatments reported so far are modest. To guide drug development, more and better-defined translational data on the pathogenesis of this severe and enigmatic inflammatory skin disease are required.

摘要

2015年肿瘤坏死因子-α抑制剂阿达木单抗的获批是化脓性汗腺炎/反向性痤疮(HS)治疗的一大重要进展。然而,很快就发现阿达木单抗在日常临床实践中的疗效差异很大。HS患者仍有重大未满足的医疗需求,因此对新型治疗靶点的探索也更加深入。在第10届欧洲化脓性汗腺炎基金会(EHSF)会议期间,知名的国际HS研究人员展示并讨论了有关这些未来HS治疗潜在靶点分子的已发表数据。本文从病理生理学和临床角度探讨了目前正在研究的最有前景的分子。随着III期试验的进行,抗白细胞介素(IL)-17生物制剂比美吉珠单抗和司库奇尤单抗正处于临床开发的最 advanced 阶段,显示出有前景的结果。此外,用贝美吉单抗靶向IL-1α在两项临床试验中已显示出令人鼓舞的结果。通过用司泊利单抗靶向IL-36来针对中性粒细胞募集和激活进行治疗符合HS的致病概念,临床II期试验结果尚未公布。与原位证据相反,补体5a(C5a)和C5a受体阻断仅在重度HS患者中显示出更大的临床益处。在HS中抑制Janus激酶(JAK)1信号传导仅在最高剂量下显示出临床疗效,这突出表明有必要仔细监测JAK抑制的安全性和疗效之间的平衡。总体而言,目前报道的所有新型治疗方法的临床疗效都较为一般。为指导药物开发开发,需要更多且定义更明确的关于这种严重且神秘的炎症性皮肤病发病机制的转化数据。

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