Department of Biomedical and Clinical Sciences, Division of Inflammation and Infection/Rheumatology, Linköping University, Linköping, Sweden.
Department of Internal Medicine, Division of Rheumatology, County Hospital Ryhov, Jönköping, Sweden.
Front Immunol. 2023 May 25;14:1187584. doi: 10.3389/fimmu.2023.1187584. eCollection 2023.
The Janus kinase (JAK)-STAT signaling pathway is relevant in both Takayasu and giant cell arteritis (GCA), and the use of JAK inhibitors (JAKi) in arthritis, psoriasis, and inflammatory bowel disease is nowadays common. Some evidence of the clinical efficacy of JAKi in GCA exists and a phase III randomized controlled trial (RCT) of upadacitinib is currently recruiting. In 2017, we started using barcitinib in a GCA patient with inadequate response to corticosteroids, and later on, we treated other 14 GCA patients with baricitinib/tofacitinib during intense follow-up. The retrospective data of these 15 individuals are here summarized. GCA was diagnosed based on the ACR criteria and/or imaging techniques combined with increased C-reactive protein (CRP) and/or erythrocyte sedimentation rate (ESR) followed by a good initial response to corticosteroids. JAKi was initiated based on inflammatory activity, with increased CRP, presumably dependent on GCA with clinical symptoms, despite unsatisfying high doses of prednisolone. The mean age at JAKi initiation was 70.1 years and the mean exposure to JAKi was 19 months. From initiation, significant reductions in CRP were seen already at 3 ( = 0.02) and 6 ( = 0.02) months. A slower decrease was observed regarding ESR at 3 ( = 0.12) and 6 ( = 0.02) months. Furthermore, the daily prednisolone doses were reduced at 3 ( = 0.02) and 6 ( = 0.004) months. No GCA relapses were observed. Two patients were affected by serious infections, but JAKi therapy was retained or reintroduced after recovery. We present encouraging observational data on JAKi in GCA in one of the hitherto largest case series with long-term follow-up. Our clinical experiences will complement the results from the awaited RCT.
Janus 激酶(JAK)-STAT 信号通路在 Takayasu 动脉炎和巨细胞动脉炎(GCA)中均相关,目前在关节炎、银屑病和炎症性肠病中常使用 JAK 抑制剂(JAKi)。已有证据表明 JAKi 在 GCA 中的临床疗效,目前正在招募 upadacitinib 的 III 期随机对照试验(RCT)。2017 年,我们开始在对皮质类固醇反应不足的 GCA 患者中使用巴利昔替尼,之后在强化随访中又用巴利昔替尼/托法替尼治疗了另外 14 例 GCA 患者。现将这 15 例患者的回顾性数据总结如下。GCA 的诊断基于 ACR 标准和/或影像学技术,同时伴有 C 反应蛋白(CRP)和/或红细胞沉降率(ESR)升高,且对皮质类固醇有良好的初始反应。JAKi 的启动基于炎症活动,CRP 升高,推测与有临床症状的 GCA 有关,尽管大剂量泼尼松治疗效果不理想。JAKi 启动时的平均年龄为 70.1 岁,JAKi 的平均暴露时间为 19 个月。从启动 JAKi 开始,CRP 在 3(=0.02)和 6(=0.02)个月时就明显降低。ESR 在 3(=0.12)和 6(=0.02)个月时下降较慢。此外,在 3(=0.02)和 6(=0.004)个月时,每日泼尼松剂量减少。未观察到 GCA 复发。有 2 例患者发生严重感染,但在恢复后保留或重新开始 JAKi 治疗。我们在迄今为止最大的系列病例之一中提供了有关 GCA 中 JAKi 的令人鼓舞的观察数据,该病例系列具有长期随访。我们的临床经验将补充即将进行的 RCT 的结果。
