SAPHO综合征的生物治疗:最新进展。

Davide Firinu, Giuseppe Murgia, Maria Maddalena Lorrai, Maria Pina Barca, Maria Monica Peralta, Paolo Emilio Manconi, Stefano R del Giacco
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引用次数: 34

摘要

滑膜炎、痤疮、脓疱病、骨质增生和骨炎(SAPHO)综合征是一种罕见且常被忽视的疾病,具有突出的皮肤和关节炎症表现。自该综合征被发现以来,许多免疫抑制药物已被用于SAPHO的治疗,结果不一。使用抗TNF-α药物作为对常规药物无反应或难治性SAPHO病例的治疗选择,证明其对骨骼,皮肤和关节表现有效。TNF-α是一种促炎细胞因子和其他细胞因子的关键调节因子,包括IL-1 β, IL-6和IL-8,参与炎症,急性期反应诱导和趋化。阿那白的IL-1抑制策略已被证明是一线和二线治疗的疗效。我们在此回顾有关SAPHO综合征患者使用生物药物的文献。此外,我们首次描述了在包括抗tnf -α和Anakinra在内的多种药物失败后,使用Ustekinumab(一种针对IL-12和IL-23的p40亚基的抗体)。这种抗il - 12/ il - 23药物可能是一种很有前途的治疗选择,也考虑到有机会干扰il - 23/TH17途径,我们最近发现该途径受到干扰。此外,使用新的抗il -1拮抗剂或IL-17抑制剂的基本原理出现了,特别是对于最难治疗的SAPHO病例。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Biological treatments for SAPHO syndrome: an update.

Synovitis, Acne, Pustulosis, Hyperostosis and Osteitis (SAPHO) syndrome is a rare and often unrecognized disease with prominent inflammatory cutaneous and articular manifestations. Since the identification of the syndrome many immunosuppressive drugs have been used for the management of SAPHO, with variable results. The use of anti- TNF-α agents as a therapeutic option for SAPHO cases unresponsive or refractory to conventional drugs, demonstrated their efficacy for bone, skin and joints manifestations. TNF-α is a pro-inflammatory cytokine and pivotal regulator of other cytokines, including IL-1 β , IL-6 and IL-8, involved in inflammation, acute-phase response induction and chemotaxis. IL-1 inhibition strategies with Anakinra have proven their efficacy as first and second line treatment. We herein review the literature concerning the use of biological drugs in patients with SAPHO syndrome. In addition, we describe for the first time the use of Ustekinumab, an antibody against the p40 subunit of IL-12 and IL-23, after failure of multiple drugs including anti-TNF-α and Anakinra. This anti-IL12/IL23 agent could be a promising therapeutic option, also considering the opportunity to interfere with the IL23/TH17 pathway, which we recently found disturbed. Furthermore, a rationale emerges for the use of the new anti-IL-1 antagonists or the IL-17 blockade, in particular for the most difficult-to-treat SAPHO cases.

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