预防类风湿关节炎的机制驱动战略。

IF 1.2 Q4 IMMUNOLOGY Rheumatology & autoimmunity Pub Date : 2022-09-01 Epub Date: 2022-06-15 DOI:10.1002/rai2.12043
V Michael Holers, Kristine A Kuhn, M Kristen Demoruelle, Jill M Norris, Gary S Firestein, Eddie A James, William H Robinson, Jane H Buckner, Kevin D Deane
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摘要

在血清反应阳性的类风湿性关节炎(RA)患者中,临床表现为炎症性关节炎(IA)的发病前通常会有一段较长的自身免疫期,表现为存在循环自身抗体,包括瓜氨酸化蛋白抗原(ACPA)和类风湿因子(RF)抗体。对于那些已发展到临床诊断为类风湿关节炎的人,临床IA之前的这段时间可被称为临床前类风湿关节炎,而对于那些尚未发展到临床IA但表现出未来临床类风湿关节炎的预测性生物标志物的人,则处于 "高危 "状态。为了制定RA预防策略,研究人员对临床前RA/高危状态的免疫表型进行了描述。从这些研究中,我们发现了一个模型,即粘膜炎症和菌群失调可能首先导致局部自身抗体的产生,这种产生通常是短暂的,但随后会导致自身免疫的全身扩散,表现为血清自身抗体升高,并最终导致临床上确定的关节炎症的发展。这一模型可被视为通过一系列 "检查点 "进行疾病发展的过程,这些检查点原则上应限制或解决自身免疫问题,然而,检查点却 "失效 "了,从而导致临床 RA 的发生。在此,我们回顾了每一步可能出现的免疫过程,以及可用于延缓、减轻、阻止甚至逆转临床RA进展的潜在治疗策略。值得注意的是,这些预防策略可以利用已获准用于临床RA的现有疗法、已获准用于其他疾病(针对临床前/风险状态下的相关途径)的疗法或针对新型途径的方法。
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Mechanism-driven strategies for prevention of rheumatoid arthritis.

In seropositive rheumatoid arthritis (RA), the onset of clinically apparent inflammatory arthritis (IA) is typically preceded by a prolonged period of autoimmunity manifest by the presence of circulating autoantibodies that can include antibodies to citrullinated protein antigens (ACPA) and rheumatoid factor (RF). This period prior to clinical IA can be designated preclinical RA in those individuals who have progressed to a clinical diagnosis of RA, and an 'at-risk' status in those who have not developed IA but exhibit predictive biomarkers of future clinical RA. With the goal of developing RA prevention strategies, studies have characterized immune phenotypes of preclinical RA/at-risk states. From these studies, a model has emerged wherein mucosal inflammation and dysbiosis may lead first to local autoantibody production that should normally be transient, but instead is followed by systemic spread of the autoimmunity as manifest by serum autoantibody elevations, and ultimately drives the development of clinically identified joint inflammation. This model can be envisioned as the progression of disease development through serial 'checkpoints' that in principle should constrain or resolve autoimmunity; however, instead the checkpoints 'fail' and clinical RA develops. Herein we review the immune processes that are likely to be present at each step and the potential therapeutic strategies that could be envisioned to delay, diminish, halt or even reverse the progression to clinical RA. Notably, these prevention strategies could utilize existing therapies approved for clinical RA, therapies approved for other diseases that target relevant pathways in the preclinical/at-risk state, or approaches that target novel pathways.

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