Universidade de Sao Paulo, Faculdade de Medicina (USP FM), Sao Paulo, Brazil.
Universidade Federal de Sao Paulo, Escola Paulista de Medicina (Unifesp EPM), Rua Otonis, 863, Vila Clementino, São Paulo, SP, 04025-002, Brazil.
Adv Rheumatol. 2024 Aug 22;64(1):62. doi: 10.1186/s42358-024-00404-9.
Systemic autoinflammatory diseases (SAIDs) arise from dysregulated innate immune system activity, which leads to systemic inflammation. These disorders, encompassing a diverse array of genetic defects classified as inborn errors of immunity, are significant diagnostic challenges due to their genetic heterogeneity and varied clinical presentations. Although recent advances in genetic sequencing have facilitated pathogenic gene discovery, approximately 40% of SAIDs patients lack molecular diagnoses. SAIDs have distinct clinical phenotypes, and targeted therapeutic approaches are needed. This review aims to underscore the complexity and clinical significance of SAIDs, focusing on prototypical disorders grouped according to their pathophysiology as follows: (i) inflammasomopathies, characterized by excessive activation of inflammasomes, which induces notable IL-1β release; (ii) relopathies, which are monogenic disorders characterized by dysregulation within the NF-κB signaling pathway; (iii) IL-18/IL-36 signaling pathway defect-induced SAIDs, autoinflammatory conditions defined by a dysregulated balance of IL-18/IL-36 cytokine signaling, leading to uncontrolled inflammation and tissue damage, mainly in the skin; (iv) type I interferonopathies, a diverse group of disorders characterized by uncontrolled production of type I interferons (IFNs), notably interferon α, β, and ε; (v) anti-inflammatory signaling pathway impairment-induced SAIDs, a spectrum of conditions characterized by IL-10 and TGFβ anti-inflammatory pathway disruption; and (vi) miscellaneous and polygenic SAIDs. The latter group includes VEXAS syndrome, chronic recurrent multifocal osteomyelitis/chronic nonbacterial osteomyelitis, Schnitzler syndrome, and Still's disease, among others, illustrating the heterogeneity of SAIDs and the difficulty in creating a comprehensive classification. Therapeutic strategies involving targeted agents, such as JAK inhibitors, IL-1 blockers, and TNF inhibitors, are tailored to the specific disease phenotypes.
自身炎症性疾病(SAIDs)源于先天免疫系统失调导致的全身炎症。这些疾病由多种遗传缺陷引起,可分类为先天性免疫缺陷,由于其遗传异质性和不同的临床表现,这些疾病具有很大的诊断挑战性。尽管遗传测序的最新进展促进了致病基因的发现,但约有 40%的 SAIDs 患者缺乏分子诊断。SAIDs 具有独特的临床表型,需要针对特定疾病的治疗方法。本综述旨在强调 SAIDs 的复杂性和临床意义,重点关注根据其病理生理学分组的典型疾病,如下:(i)炎症小体病,其特征是炎症小体过度激活,导致明显的 IL-1β 释放;(ii)Relopathies,是由 NF-κB 信号通路失调引起的单基因疾病;(iii)IL-18/IL-36 信号通路缺陷引起的 SAIDs,是由 IL-18/IL-36 细胞因子信号失衡引起的自身炎症性疾病,导致不受控制的炎症和组织损伤,主要发生在皮肤;(iv)I 型干扰素病,是一组由 I 型干扰素(IFN)失控产生引起的多种疾病,特别是干扰素 α、β 和 ε;(v)抗炎信号通路缺陷引起的 SAIDs,是一组由 IL-10 和 TGFβ 抗炎通路破坏引起的疾病;(vi)杂合性和多基因性 SAIDs。后者包括 VEXAS 综合征、慢性复发性多灶性骨炎/慢性非细菌性骨髓炎、 Schnitzler 综合征和斯蒂尔病等,说明了 SAIDs 的异质性和创建全面分类的困难。靶向治疗策略,如 JAK 抑制剂、IL-1 阻滞剂和 TNF 抑制剂,根据特定的疾病表型进行定制。
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