Division of Immunology, Boston Children's Hospital, Boston, Massachusetts.
Division of Rheumatology, Inflammation, and Immunity, Brigham and Women's Hospital, Boston, Massachusetts.
Arthritis Rheumatol. 2022 Nov;74(11):1851-1858. doi: 10.1002/art.42240. Epub 2022 Sep 30.
Inflammatory arthritides exhibit hallmark patterns of affected and spared joints, but in each individual, arthritis affects only a subset of all possible sites. The purpose of this study was to identify patient-specific patterns of joint flare to distinguish local from systemic drivers of disease chronicity.
Patients with juvenile idiopathic arthritis followed without interruption from disease onset into adulthood were identified across 2 large academic centers. Joints inflamed at each visit were established by medical record review. Flare was defined as physician-confirmed joint inflammation following documented inactive disease.
Among 222 adults with JIA, 95 had complete serial joint examinations dating from disease onset in childhood. Mean follow-up was 12.5 years (interquartile range 7.9-16.7 years). Ninety (95%) of 95 patients achieved inactive disease, after which 81% (73 patients) experienced at least 1 flare. Among 940 joints affected in 253 flares, 74% had been involved previously. In flares affecting easily observed large joint pairs where only 1 side had been involved before (n = 53), the original joint was affected in 83% and the contralateral joint in 17% (P < 0.0001 versus random laterality). However, disease extended to at least 1 new joint in ~40% of flares, a risk that remained stable even decades after disease onset, and was greatest in flares that occurred while patients were not receiving medication (54% versus 36% of flares occurring with therapy; odds ratio 2.09, P = 0.015).
Arthritis flares preferentially affect previously inflamed joints but carry an ongoing risk of disease extension. These findings confirm joint-specific memory and suggest that prevention of new joint accumulation should be an important target for arthritis therapy.
炎症性关节炎表现出受影响和未受影响关节的典型模式,但在每个个体中,关节炎仅影响所有可能部位的一部分。本研究的目的是确定患者特定的关节发作模式,以区分疾病慢性化的局部和全身驱动因素。
在 2 个大型学术中心中,确定了从发病开始一直不间断地随访到成年的幼年特发性关节炎患者。通过病历回顾确定每次就诊时发炎的关节。发作定义为经医生确认的疾病静止期后出现的关节炎症。
在 222 名患有 JIA 的成年人中,有 95 名患者的完整连续关节检查可追溯到儿童时期发病。平均随访时间为 12.5 年(四分位距 7.9-16.7 年)。95 名患者中有 90 名(95%)达到疾病静止期,此后 81%(73 名患者)至少经历过 1 次发作。在 253 次发作中影响的 940 个关节中,74%以前曾受累。在影响易于观察的大关节对且以前只有 1 侧受累的 53 次发作中,原始关节受累率为 83%,对侧关节受累率为 17%(P<0.0001 与随机侧别相比)。然而,即使在发病几十年后,疾病仍会扩展到至少 1 个新关节,这种风险仍然稳定,并且在患者未接受药物治疗时发作的风险最高(54%与治疗中发作的 36%相比;比值比 2.09,P=0.015)。
关节炎发作优先影响以前发炎的关节,但仍存在疾病扩展的风险。这些发现证实了关节特异性记忆,并表明预防新关节积累应该是关节炎治疗的一个重要目标。