Department of Clinical Immunology and Rheumatology, Christian Medical College, Vellore 632004, India.
Department of Clinical Immunology and Rheumatology, Christian Medical College, Vellore 632004, India.
Semin Arthritis Rheum. 2018 Apr;47(5):718-726. doi: 10.1016/j.semarthrit.2017.09.014. Epub 2017 Sep 30.
Long-term outcome studies in Takayasu arteritis (TA) are few and limited by small sample size. In this study, we analysed the outcome of treatment in a large series of TA patients with a minimum follow-up period of ≥12 months by objective instruments.
Patients with TA satisfying the 1990 ACR, Ishikawa's, Sharma's or EULAR/PRESS criteria were recruited from our clinics between 1998 and 2016. Only patients with a minimum follow up of 12 months were studied. Data related to clinical presentation, disease extent (DEI.Tak score), activity [Indian Takayasu arteritis clinical activity score, that is, ITAS-A (CRP)] and damage score [Takayasu arteritis damage score (TADS)], angiography and treatment were collected for all patients. Response to treatment was categorised as complete response (CR), partial response (PR) or refractory disease. Patients with sustained CR on prednisolone dose of ≤5mg/day were classified as having sustained inactive disease. Appropriate statistical tests were used for parametric and non-parametric data. Relapse free survival was projected by Kaplan-Meir curve. Cox proportional hazards regression plot was used to compare the efficacy of medications. Predictors of sustained response were identified by logistic regression and a prediction model was constructed.
Among 503 TA patients examined during study period, 251 had follow-up of ≥12 months and were included in this study. Median follow-up duration was 42 months (IQR: 24-81, maximum 240 months). Patients (81.7% females, mean age of 29.2 ± 11.8 years, symptom duration of 24 [6-70] months) were treated by a uniform protocol that included high dose steroids (n = 239) plus concurrent steroid-sparing immunosuppressant (n = 235) with mycophenolate in majority. Biological agents (n = 44 patients) and revascularisation procedures were used in symptomatic patients after control of disease activity. At 1st follow-up, CR (ITAS2010 = 0, CRP < 6mg/L and non-progressive disease on angiography) was observed in 173 (68.9%), partial response (PR) in 42 (16.7%) and no response was seen in only 36 (14%) patients. CR was sustained till the last follow up in 116 (65.9%) of 173 patients with initial CR, while 87 (49.4%) of them achieved sustained inactive disease. Disease activity relapsed at a median duration of 37 (29.9-44.1) months in 56 patients. Cumulative relapse free survival was 93%, 73%, 66% and 52% at 1, 3, 5 and 10 years, respectively. Baseline CRP < 6.2, DEI.Tak < 9 and angiographic type 4 disease predicted sustained inactive disease and a model comprising these parameters showed sensitivity and specificity of 70% and 61.1%. Two fatalities were observed. New vascular lesions during follow up were observed in 50 (19.9%) patients. Overall, 92.8% had at least one period of CR or PR while 7.2% were refractory to treatment till the last follow up. Damage progression (∆TADS > 1) was arrested in 68% of patients and was lower in patients with sustained inactive disease [0 (0-1)] as compared to the rest [1 (0-2.75)], p = 0.000. Both early response as well as cumulative hazard for relapse were similar between patients initiated on 0.5 and 1mg/kg/day steroids.
Our strategy of upfront combination immunosuppressant therapy stabilised disease activity in 92.8% of patients, while 7.2% had true refractory disease. Relapse free survival was 66% at 5 years and 52% at 10 years. Damage progression was arrested in 68% and only 2 fatalities were observed. Initial steroid dose of 0.5mg/kg/day had similar efficacy as 1mg/kg/day dose.
在多发性大动脉炎(TA)中,长期预后研究较少且受到样本量小的限制。在这项研究中,我们通过客观的仪器分析了满足 1990 年 ACR、Ishikawa's、Sharma's 或 EULAR/PRESS 标准的大量 TA 患者在至少 12 个月的随访期内的治疗结果。
1998 年至 2016 年期间,我们从诊所招募了满足 1990 年 ACR、Ishikawa's、Sharma's 或 EULAR/PRESS 标准的 TA 患者。仅对随访时间至少为 12 个月的患者进行研究。收集了所有患者的临床症状、疾病范围(DEI.Tak 评分)、活动度[印度 Takayasu 动脉炎临床活动评分,即 ITAS-A(CRP)]和损伤评分[Takayasu 动脉炎损伤评分(TADS)]、血管造影和治疗的相关数据。将治疗反应分为完全反应(CR)、部分反应(PR)或难治性疾病。对泼尼松剂量≤5mg/天的患者,将其持续 CR 归类为持续无活动性病。对参数和非参数数据进行了适当的统计检验。通过 Kaplan-Meier 曲线预测无复发生存率。使用 Cox 比例风险回归图比较药物的疗效。通过逻辑回归识别持续反应的预测因素,并构建预测模型。
在研究期间检查的 503 例 TA 患者中,251 例有≥12 个月的随访并纳入本研究。中位随访时间为 42 个月(IQR:24-81,最大 240 个月)。患者(81.7%为女性,平均年龄 29.2±11.8 岁,症状持续时间 24[6-70]个月)接受了统一的治疗方案,包括高剂量类固醇(n=239)联合同时使用类固醇的免疫抑制剂(n=235),其中大多数使用的是霉酚酸酯。在疾病活动得到控制后,有症状的患者使用生物制剂(n=44 例)和血管重建术。在第一次随访时,173 例患者(68.9%)达到了 CR(ITAS2010=0,CRP<6mg/L 和血管造影无进展性疾病),42 例患者(16.7%)达到了 PR,36 例患者(14%)无反应。在最初达到 CR 的 173 例患者中,116 例(65.9%)患者的 CR 持续到最后一次随访,其中 87 例(49.4%)患者达到了持续的无活动性病。56 例患者在中位时间 37(29.9-44.1)个月时疾病活动复发。在 1、3、5 和 10 年时,无复发生存率分别为 93%、73%、66%和 52%。基线 CRP<6.2、DEI.Tak<9 和血管造影 4 型疾病预测持续无活动性病,包含这些参数的模型显示了 70%的敏感性和 61.1%的特异性。观察到 2 例死亡。在随访期间,50 例(19.9%)患者出现新的血管病变。总的来说,92.8%的患者至少有一个时期的 CR 或 PR,而 7.2%的患者直到最后一次随访仍对治疗有反应。68%的患者的损伤进展(∆TADS>1)得到了控制,持续无活动性病患者的损伤进展[0(0-1)]低于其余患者[1(0-2.75)],p=0.000。在起始剂量为 0.5 和 1mg/kg/天的患者中,早期反应和累积复发的危险度相似。
我们的一线联合免疫抑制剂治疗策略稳定了 92.8%的患者的疾病活动度,而 7.2%的患者为真正的难治性疾病。5 年和 10 年的无复发生存率分别为 66%和 52%。损伤进展得到了控制,有 68%的患者,仅观察到 2 例死亡。起始剂量为 0.5mg/kg/天的泼尼松与 1mg/kg/天的剂量疗效相似。
