New and future perspectives in familial Mediterranean fever and other autoinflammatory diseases.

IF 1.1 Q4 RHEUMATOLOGY
Archives of rheumatology Pub Date : 2024-08-26 eCollection Date: 2024-09-01 DOI:10.46497/ArchRheumatol.2024.10911
Veysel Çam, Hülya Ercan Emreol, Seza Ozen
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Abstract

Systemic autoinflammatory diseases are a group of disorders characterized by sterile episodes of inflammation resulting from defects in the innate immune system. In contrast to classical autoimmune diseases, where circulating autoantibodies and the adaptive immune system are involved, these conditions involve excessive presence of proinflammatory cytokines leading to inflammatory attacks. Excessive cytokine production, functional mutations in regulatory pathways, excessive interferon production, defects in the nuclear factor-kappa B signaling pathway, abnorARCHmal protein folding, and complement activation are the mechanisms leading to autoinflammatory diseases. A defect in the mTOR pathway and trained immunity are newly discovered possible causes in pathogenesis. Early onset and severe forms of classical rheumatological diseases have been more frequently associated with autoinflammatory diseases in the last decade. Therefore, monogenic autoinflammatory diseases should be considered in rheumatic diseases with family history, consanguinity, early onset, and severe disease. The combination of functional and genotyping research will help to identify unclassified patients. The optimal treatment strategy remains uncertain, functional studies such as interferon signature and cytokine profiling, may prove valuable in guiding the treatment process. Stem cell transplantation strategies in autoinflammatory diseases with partial response to biological therapies can be considered. Autoinflammatory diseases are becoming increasingly complex and are bringing new perspectives to already known rheumatic diseases. Although we have effective treatments, we are still far from personalized recommendations.

家族性地中海热和其他自身炎症性疾病的新前景和未来展望。
全身性自身炎症性疾病是一组以先天性免疫系统缺陷导致的无菌性炎症发作为特征的疾病。与涉及循环自身抗体和适应性免疫系统的传统自身免疫性疾病不同,这些疾病涉及促炎细胞因子的过度存在,从而导致炎症发作。导致自身炎症性疾病的机制包括细胞因子产生过多、调控通路发生功能性突变、干扰素产生过多、核因子-kappa B 信号通路缺陷、蛋白质折叠异常和补体激活。mTOR 通路的缺陷和训练有素的免疫力是新发现的可能致病原因。近十年来,早发和严重形式的经典风湿病越来越多地与自身炎症性疾病相关。因此,对于有家族史、近亲结婚、早发和病情严重的风湿病,应考虑单基因自身炎症性疾病。功能研究和基因分型研究的结合将有助于识别未分类的患者。最佳治疗策略仍不确定,但干扰素特征和细胞因子图谱等功能研究可能对指导治疗过程很有价值。对于对生物疗法有部分反应的自身炎症性疾病,可以考虑干细胞移植策略。自身炎症性疾病正变得越来越复杂,为已知的风湿性疾病带来了新的视角。虽然我们已经有了有效的治疗方法,但离个性化建议还很遥远。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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